Compositions for the treatment and diagnosis of breast cancer and methods for their use

ABSTRACT

Compounds and methods for the treatment and diagnosis of breast cancer are provided. The inventive compounds include polypeptides containing at least a portion of a breast tumor antigen. Vaccines and pharmaceutical compositions for immunotherapy of breast cancer comprising such polypeptides, or polynucleotides encoding such polypeptides, are provided, together with polynucleotides for preparing the inventive polypeptides. The inventive polypeptides may be used to generate antibodies useful for the diagnosis and monitoring of breast cancer.

CROSS-REFERENCE TO RELATED APPLICATIONS

[0001] This application is a continuation-in-part of U.S. application Ser. No. 09/222,575, filed Dec. 28, 1998.

TECHNICAL FIELD

[0002] The present invention relates generally to compositions and methods for the treatment of breast cancer. The invention is more particularly related to polypeptides comprising at least a portion of a protein that is preferentially expressed in breast tumor tissue and to polynucleotides encoding such polypeptides. Such polypeptides and polynucleotides may be used in vaccines and pharmaceutical compositions for treatment of breast cancer.

BACKGROUND OF THE INVENTION

[0003] Breast cancer is a significant health problem for women in the United States and throughout the world. Although advances have been made in detection and treatment of the disease, breast cancer remains the second leading cause of cancer-related deaths in women, affecting more than 180,000 women in the United States each year. For women in North America, the life-time odds of getting breast cancer are one in eight.

[0004] No vaccine or other universally successful method for the prevention or treatment of breast cancer is currently available. Management of the disease currently relies on a combination of early diagnosis (through routine breast screening procedures) and aggressive treatment, which may include one or more of a variety of treatments such as surgery, radiotherapy, chemotherapy and hormone therapy. The course of treatment for a particular breast cancer is often selected based on a variety of prognostic parameters, including an analysis of specific tumor markers. See, e.g., Porter-Jordan and Lippman, Breast Cancer 8:73-100 (1994). However, the use of established markers often leads to a result that is difficult to interpret, and the high mortality observed in breast cancer patients indicates that improvements are needed in the treatment, diagnosis and prevention of the disease.

[0005] Accordingly, there is a need in the art for improved methods for the treatment and diagnosis of breast cancer. The present invention fulfills these needs and further provides other related advantages.

SUMMARY OF THE INVENTION

[0006] The present invention provides compounds and methods for the treatment and diagnosis of breast cancer. In one aspect, isolated polypeptides are provided comprising at least an immunogenic portion of a breast tumor antigen or a variant thereof, wherein the antigen comprises an amino acid sequence encoded by a polynucleotide having a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions. In specific embodiments, the inventive polypeptides comprise an amino acid sequence selected from the group consisting of SEQ ID NO: 62, 176, 179 and 181.

[0007] In related aspects, isolated polynucleotides encoding the above polypeptides are provided. In specific embodiments, such polynucleotides comprise a sequence selected from the group consisting of sequences provided in SEQ ID NO: 1-61, 63-175, 178 and 180. The present invention further provides expression vectors comprising the above polynucleotides, together with host cells transformed or transfected with such expression vectors. In preferred embodiments, the host cells are selected from the group consisting of E coli, yeast and mammalian cells.

[0008] In another aspect, the present invention provides fusion proteins comprising a first and a second inventive polypeptide or, alternatively, an inventive polypeptide and a known breast tumor antigen.

[0009] The present invention also provides pharmaceutical compositions comprising at least one of the above polypeptides, or a polynucleotide encoding such a polypeptide, and a physiologically acceptable carrier, together with vaccines comprising at least one such polypeptide or polynucleotide in combination with a non-specific immune response enhancer. Pharmaceutical compositions and vaccines comprising one or more of the above fusion proteins are also provided.

[0010] In yet another aspect, methods are provided for inhibiting the development of breast cancer in a patient, comprising administering an effective amount of at least one of the above pharmaceutical compositions and/or vaccines.

[0011] The polypeptides disclosed herein may be usefully employed in the diagnosis and monitoring of breast cancer. In one aspect of the present invention, methods are provided for detecting breast cancer in a patient, comprising: (a) contacting a biological sample obtained from a patient with a binding agent that is capable of binding to one of the above polypeptides; and (b) detecting in the sample a protein or polypeptide that binds to the binding agent. In preferred embodiments, the binding agent is an antibody, most preferably a monoclonal antibody.

[0012] In related aspects, methods are provided for monitoring the progression of breast cancer in a patient, comprising: (a) contacting a biological sample obtained from a patient with a binding agent that is capable of binding to one of the above polypeptides; (b) determining in the sample an amount of a protein or polypeptide that binds to the binding agent; (c) repeating steps (a) and (b); and comparing the amounts of polypeptide detected in steps (b) and (c).

[0013] Within related aspects, the present invention provides antibodies, preferably monoclonal antibodies, that bind to the inventive polypeptides, as well as diagnostic kits comprising such antibodies, and methods of using such antibodies to inhibit the development of breast cancer.

[0014] The present invention further provides methods for detecting breast cancer comprising: (a) obtaining a biological sample from a patient; (b) contacting the sample with a first and a second oligonucleotide primer in a polymerase chain reaction, at least one of the oligonucleotide primers being specific for a polynucleotide that encodes one of the above polypeptides; and (c) detecting in the sample a DNA sequence that amplifies in the presence of the first and second oligonucleotide primers. In a preferred embodiment, at least one of the oligonucleotide primers comprises at least about 10 contiguous nucleotides of a polynucleotide comprising a sequence selected from the group consisting of SEQ ID NO: 1-61, 63-175, 178 and 180.

[0015] In a further aspect, the present invention provides a method for detecting breast cancer in a patient comprising: (a) obtaining a biological sample from the patient; (b) contacting the sample with an oligonucleotide probe specific for a polynucleotide that encodes one of the above polypeptides; and (c) detecting in the sample a DNA sequence that hybridizes to the oligonucleotide probe. Preferably, the oligonucleotide probe comprises at least about 15 contiguous nucleotides of a polynucleotide comprising a sequence selected from the group consisting of SEQ ID NO: 1-61, 63-175, 178 and 180.

[0016] In related aspects, diagnostic kits comprising the above oligonucleotide probes or primers are provided.

[0017] These and other aspects of the present invention will become apparent upon reference to the following detailed description. All references disclosed herein are hereby incorporated by reference in their entirety as if each was incorporated individually.

BRIEF DESCRIPTION OF THE DRAWING AND SEQUENCE IDENTIFIERS

[0018]FIG. 1 shows the results of a Northern blot of the clone SYN18C6 (SEQ ID NO: 40).

[0019] SEQ ID NO: 1 is the determined cDNA sequence of JBT2.

[0020] SEQ ID NO: 2 is the determined cDNA sequence of JBT6.

[0021] SEQ ID NO: 3 is the determined cDNA sequence of JBT7.

[0022] SEQ ID NO: 4 is the determined cDNA sequence of JBT10.

[0023] SEQ ID NO: 5 is the determined cDNA sequence of JBT13.

[0024] SEQ ID NO: 6 is the determined cDNA sequence of JBT14.

[0025] SEQ ID NO: 7 is the determined cDNA sequence of JBT15.

[0026] SEQ ID NO: 8 is the determined cDNA sequence of JBT16.

[0027] SEQ ID NO: 9 is the determined cDNA sequence of JBT17.

[0028] SEQ ID NO: 10 is the determined cDNA sequence of JBT22.

[0029] SEQ ID NO: 11 is the determined cDNA sequence of JBT25.

[0030] SEQ ID NO: 12 is the determined cDNA sequence of JBT28.

[0031] SEQ ID NO: 13 is the determined cDNA sequence of JBT32.

[0032] SEQ ID NO: 14 is the determined cDNA sequence of JBT33.

[0033] SEQ ID NO: 15 is the determined cDNA sequence of JBT34.

[0034] SEQ ID NO: 16 is the determined cDNA sequence of JBT36.

[0035] SEQ ID NO: 17 is the determined cDNA sequence of JBT37.

[0036] SEQ ID NO: 18 is the determined cDNA sequence of JBT51.

[0037] SEQ ID NO: 19 is the determined cDNA sequence of JBTT1.

[0038] SEQ ID NO: 20 is the determined cDNA sequence of JBTT7.

[0039] SEQ ID NO: 21 is the determined cDNA sequence of JBTT11.

[0040] SEQ ID NO: 22 is the determined cDNA sequence of JBTT14.

[0041] SEQ ID NO: 23 is the determined cDNA sequence of JBTT18.

[0042] SEQ ID NO: 24 is the determined cDNA sequence of JBTT19.

[0043] SEQ ID NO: 25 is the determined cDNA sequence of JBTT20.

[0044] SEQ ID NO: 26 is the determined cDNA sequence of JBTT21.

[0045] SEQ ID NO: 27 is the determined cDNA sequence of JBTT22.

[0046] SEQ ID NO: 28 is the determined cDNA sequence of JBTT28.

[0047] SEQ ID NO: 29 is the determined cDNA sequence of JBTT29.

[0048] SEQ ID NO: 30 is the determined cDNA sequence of JBTT33.

[0049] SEQ ID NO: 31 is the determined cDNA sequence of JBTT37.

[0050] SEQ ID NO: 32 is the determined cDNA sequence of JBTT38.

[0051] SEQ ID NO: 33 is the determined cDNA sequence of JBTT47.

[0052] SEQ ID NO: 34 is the determined cDNA sequence of JBTT48.

[0053] SEQ ID NO: 35 is the determined cDNA sequence of JBTT50.

[0054] SEQ ID NO: 36 is the determined cDNA sequence of JBTT51.

[0055] SEQ ID NO: 37 is the determined cDNA sequence of JBTT52.

[0056] SEQ ID NO: 38 is the determined cDNA sequence of JBTT54.

[0057] SEQ ID NO: 39 is the determined cDNA sequence of SYN17F4.

[0058] SEQ ID NO: 40 is the determined cDNA sequence of SYN18C6.

[0059] SEQ ID NO: 41 is the determined cDNA sequence of SYN19A2.

[0060] SEQ ID NO: 42 is the determined cDNA sequence of SYN19C8.

[0061] SEQ ID NO: 43 is the determined cDNA sequence of SYN20A12.

[0062] SEQ ID NO: 44 is the determined cDNA sequence of SYN20G6.

[0063] SEQ ID NO: 45 is the determined cDNA sequence of SYN20G6-2.

[0064] SEQ ID NO: 46 is the determined cDNA sequence of SYN21B9.

[0065] SEQ ID NO: 47 is the determined cDNA sequence of SYN21B9-2.

[0066] SEQ ID NO: 48 is the determined cDNA sequence of SYN21C10.

[0067] SEQ ID NO: 49 is the determined cDNA sequence of SYN21G10.

[0068] SEQ ID NO: 50 is the determined cDNA sequence of SYN21G10-2.

[0069] SEQ ID NO: 51 is the determined cDNA sequence of SYN21G11.

[0070] SEQ ID NO: 52 is the determined cDNA sequence of SYN21G11-2.

[0071] SEQ ID NO: 53 is the determined cDNA sequence of SYN21H8.

[0072] SEQ ID NO: 54 is the determined cDNA sequence of SYN22A10.

[0073] SEQ ID NO: 55 is the determined cDNA sequence of SYN22A10-2.

[0074] SEQ ID NO: 56 is the determined cDNA sequence of SYN22A12.

[0075] SEQ ID NO: 57 is the determined cDNA sequence of SYN22A2.

[0076] SEQ ID NO: 58 is the determined cDNA sequence of SYN22B4.

[0077] SEQ ID NO: 59 is the determined cDNA sequence of SYN22C2.

[0078] SEQ ID NO: 60 is the determined cDNA sequence of SYN22E10.

[0079] SEQ ID NO: 61 is the determined cDNA sequence of SYN22F2.

[0080] SEQ ID NO: 62 is a predicted amino acid sequence for SYN18C6.

[0081] SEQ ID NO: 63 is the determined cDNA sequence of B723P.

[0082] SEQ ID NO: 64 is the determined cDNA sequence for B724P.

[0083] SEQ ID NO: 65 is the determined cDNA sequence of B770P.

[0084] SEQ ID NO: 66 is the determined cDNA sequence of B716P.

[0085] SEQ ID NO: 67 is the determined cDNA sequence of B725P.

[0086] SEQ ID NO: 68 is the determined cDNA sequence of B717P.

[0087] SEQ ID NO: 69 is the determined cDNA sequence of B771P.

[0088] SEQ ID NO: 70 is the determined cDNA sequence of B722P.

[0089] SEQ ID NO: 71 is the determined cDNA sequence of B726P.

[0090] SEQ ID NO: 72 is the determined cDNA sequence of B727P.

[0091] SEQ ID NO: 73 is the determined cDNA sequence of B728P.

[0092] SEQ ID NO: 74-87 are the determined cDNA sequences of isolated clones which show homology to known sequences.

[0093] SEQ ID NO: 88 is the determined cDNA sequence of 13053.

[0094] SEQ ID NO: 89 is the determined cDNA sequence of 13057.

[0095] SEQ ID NO: 90 is the determined cDNA sequence of 13059.

[0096] SEQ ID NO: 91 is the determined cDNA sequence of 13065.

[0097] SEQ ID NO: 92 is the determined cDNA sequence of 13067.

[0098] SEQ ID NO: 93 is the determined cDNA sequence of 13068.

[0099] SEQ ID NO: 94 is the determined cDNA sequence of 13071.

[0100] SEQ ID NO: 95 is the determined cDNA sequence of 13072.

[0101] SEQ ID NO: 96 is the determined cDNA sequence of 13073.

[0102] SEQ ID NO: 97 is the determined cDNA sequence of 13075.

[0103] SEQ ID NO: 98 is the determined cDNA sequence of 13078.

[0104] SEQ ID NO: 99 is the determined cDNA sequence of 13079.

[0105] SEQ ID NO: 100 is the determined cDNA sequence of 13081.

[0106] SEQ ID NO: 101 is the determined cDNA sequence of 13082.

[0107] SEQ ID NO: 102 is the determined cDNA sequence of 13092.

[0108] SEQ ID NO: 103 is the determined cDNA sequence of 13097.

[0109] SEQ ID NO: 104 is the determined cDNA sequence of 13101.

[0110] SEQ ID NO: 105 is the determined cDNA sequence of 13102.

[0111] SEQ ID NO: 106 is the determined cDNA sequence of 13119.

[0112] SEQ ID NO: 107 is the determined cDNA sequence of 13131.

[0113] SEQ ID NO: 108 is the determined cDNA sequence of 13133.

[0114] SEQ ID NO: 109 is the determined cDNA sequence of 13135.

[0115] SEQ ID NO: 110 is the determined cDNA sequence of 13139.

[0116] SEQ ID NO: 111 is the determined cDNA sequence of 13140.

[0117] SEQ ID NO: 112 is the determined cDNA sequence of 13146.

[0118] SEQ ID NO: 113 is the determined cDNA sequence of 13147.

[0119] SEQ ID NO: 114 is the determined cDNA sequence of 13148.

[0120] SEQ ID NO: 115 is the determined cDNA sequence of 13149.

[0121] SEQ ID NO: 116 is the determined cDNA sequence of 13151.

[0122] SEQ ID NO: 117 is the determined cDNA sequence of 13051

[0123] SEQ ID NO: 118 is the determined cDNA sequence of 13052

[0124] SEQ ID NO: 119 is the determined cDNA sequence of 13055

[0125] SEQ ID NO: 120 is the determined cDNA sequence of 13058

[0126] SEQ ID NO: 121 is the determined cDNA sequence of 13062

[0127] SEQ ID NO: 122 is the determined cDNA sequence of 13064

[0128] SEQ ID NO: 123 is the determined cDNA sequence of 13080

[0129] SEQ ID NO: 124 is the determined cDNA sequence of 13093

[0130] SEQ ID NO: 125 is the determined cDNA sequence of 13094

[0131] SEQ ID NO: 126 is the determined cDNA sequence of 13095

[0132] SEQ ID NO: 127 is the determined cDNA sequence of 13096

[0133] SEQ ID NO: 128 is the determined cDNA sequence of 13099

[0134] SEQ ID NO: 129 is the determined cDNA sequence of 13100

[0135] SEQ ID NO: 130 is the determined cDNA sequence of 13103

[0136] SEQ ID NO: 131 is the determined cDNA sequence of 13106

[0137] SEQ ID NO: 132 is the determined cDNA sequence of 13107

[0138] SEQ ID NO: 133 is the determined cDNA sequence of 13108

[0139] SEQ ID NO: 134 is the determined cDNA sequence of 13121

[0140] SEQ ID NO: 135 is the determined cDNA sequence of 13126

[0141] SEQ ID NO: 136 is the determined cDNA sequence of 13129

[0142] SEQ ID NO: 137 is the determined cDNA sequence of 13130

[0143] SEQ ID NO: 138 is the determined cDNA sequence of 13134

[0144] SEQ ID NO: 139 is the determined cDNA sequence of 13141

[0145] SEQ ID NO: 140 is the determined cDNA sequence of 13142

[0146] SEQ ID NO: 141 is the determined cDNA sequence of 14376

[0147] SEQ ID NO: 142 is the determined cDNA sequence of 14377

[0148] SEQ ID NO: 143 is the determined cDNA sequence of 14383

[0149] SEQ ID NO: 144 is the determined cDNA sequence of 14384

[0150] SEQ ID NO: 145 is the determined cDNA sequence of 14387

[0151] SEQ ID NO: 146 is the determined cDNA sequence of 14392

[0152] SEQ ID NO: 147 is the determined cDNA sequence of 14394

[0153] SEQ ID NO: 148 is the determined cDNA sequence of 14398

[0154] SEQ ID NO: 149 is the determined cDNA sequence of 14401

[0155] SEQ ID NO: 150 is the determined cDNA sequence of 14402

[0156] SEQ ID NO: 151 is the determined cDNA sequence of 14405

[0157] SEQ ID NO: 152 is the determined cDNA sequence of 14409

[0158] SEQ ID NO: 153 is the determined cDNA sequence of 14412

[0159] SEQ ID NO: 154 is the determined cDNA sequence of 14414

[0160] SEQ ID NO: 155 is the determined cDNA sequence of 14415

[0161] SEQ ID NO: 156 is the determined cDNA sequence of 14416

[0162] SEQ ID NO: 157 is the determined cDNA sequence of 14419

[0163] SEQ ID NO: 158 is the determined cDNA sequence of 14426

[0164] SEQ ID NO: 159 is the determined cDNA sequence of 14427

[0165] SEQ ID NO: 160 is the determined cDNA sequence of 14375

[0166] SEQ ID NO: 161 is the determined cDNA sequence of 14378

[0167] SEQ ID NO: 162 is the determined cDNA sequence of 14379

[0168] SEQ ID NO: 163 is the determined cDNA sequence of 14380

[0169] SEQ ID NO: 164 is the determined cDNA sequence of 14381

[0170] SEQ ID NO: 165 is the determined cDNA sequence of 14382

[0171] SEQ ID NO: 166 is the determined cDNA sequence of 14388

[0172] SEQ ID NO: 167 is the determined cDNA sequence of 14399

[0173] SEQ ID NO: 168 is the determined cDNA sequence of 14406

[0174] SEQ ID NO: 169 is the determined cDNA sequence of 14407

[0175] SEQ ID NO: 170 is the determined cDNA sequence of 14408

[0176] SEQ ID NO: 171 is the determined cDNA sequence of 14417

[0177] SEQ ID NO: 172 is the determined cDNA sequence of 14418

[0178] SEQ ID NO: 173 is the determined cDNA sequence of 14423

[0179] SEQ ID NO: 174 is the determined cDNA sequence of 14424

[0180] SEQ ID NO: 175 is the determined cDNA sequence of B726P-20

[0181] SEQ ID NO: 176 is the predicted amino acid sequence of B726P-20

[0182] SEQ ID NO: 177 is a PCR primer

[0183] SEQ ID NO: 178 is the determined cDNA sequence of B726P-74

[0184] SEQ ID NO: 179 is the predicted amino acid sequence of B726P-74

[0185] SEQ ID NO: 180 is the determined cDNA sequence of B726P-79

[0186] SEQ ID NO: 181 is the predicted amino acid sequence of B726P-79

DETAILED DESCRIPTION OF THE INVENTION

[0187] As noted above, the present invention is generally directed to compositions and methods for the treatment and diagnosis of breast cancer. The inventive compositions are generally isolated polypeptides that comprise at least a portion of a breast tumor antigen. Also included within the present invention are molecules (such as an antibody or fragment thereof) that bind to the inventive polypeptides. Such molecules are referred to herein as “binding agents.” In particular, the subject invention discloses polypeptides comprising at least a portion of a human breast tumor antigen, or a variant thereof, wherein the breast tumor antigen includes an amino acid sequence encoded by a polynucleotide including a sequence selected from the group consisting of: nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, the complements of said nucleotide sequences, and variants thereof. As used herein, the term “polypeptide” encompasses amino acid chains of any length, including full length proteins, wherein the amino acid residues are linked by covalent peptide bonds. Thus, a polypeptide comprising a portion of one of the above breast antigens may consist entirely of the portion, or the portion may be present within a larger polypeptide that contains additional sequences. The additional sequences may be derived from the native protein or may be heterologous, and such sequences may be immunoreactive and/or antigenic.

[0188] As used herein, an “immunogenic portion” of a human breast tumor antigen is a portion that is capable of eliciting an immune response in a patient inflicted with breast cancer and as such binds to antibodies present within sera from a breast cancer patient. Such immunogenic portions generally comprise at least about 5 amino acid residues, more preferably at least about 10, and most preferably at least about 20 amino acid residues. Immunogenic portions of the proteins described herein may be identified in antibody binding assays. Such assays may generally be performed using any of a variety of means known to those of ordinary skill in the art, as described, for example, in Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, Cold Spring Harbor, N.Y., 1988. For example, a polypeptide may be immobilized on a solid support (as described below) and contacted with patient sera to allow binding of antibodies within the sera to the immobilized polypeptide. Unbound sera may then be removed and bound antibodies detected using, for example, ¹²⁵I-labeled Protein A. Alternatively, a polypeptide may be used to generate monoclonal and polyclonal antibodies for use in detection of the polypeptide in blood or other fluids of breast cancer patients. Methods for preparing and identifying immunogenic portions of antigens of known sequence are well known in the art and include those summarized in Paul, Fundamental Immunology, 3^(rd) ed., Raven Press, 1993, pp. 243-247.

[0189] The term “polynucleotide(s),” as used herein, means a single or double-stranded polymer of deoxyribonucleotide or ribonucleotide bases and includes DNA and corresponding RNA molecules, including HnRNA and mRNA molecules, both sense and anti-sense strands, and comprehends cDNA, genomic DNA and recombinant DNA, as well as wholly or partially synthesized polynucleotides. An HnRNA molecule contains introns and corresponds to a polynucleotide in a generally one-to-one manner. An mRNA molecule corresponds to an HnRNA and polynucleotide from which the introns have been excised. A polynucleotide may consist of an entire gene, or any portion thereof. Operable anti-sense polynucleotides may comprise a fragment of the corresponding polynucleotide, and the definition of “polynucleotide” therefore includes all such operable anti-sense fragments.

[0190] The compositions and methods of the present invention also encompass variants of the above polypeptides and polynucleotides. Such variants include, but are not limited to, naturally occurring allelic variants of the inventive sequences.

[0191] A polypeptide “variant,” as used herein, is a polypeptide that differs from the recited polypeptide only in conservative substitutions and/or modifications, such that the antigenic properties of the polypeptide are retained. In a preferred embodiment, variant polypeptides differ from an identified sequence by substitution, deletion or addition of five amino acids or fewer. Such variants may generally be identified by modifying one of the above polypeptide sequences, and evaluating the antigenic properties of the modified polypeptide using, for example, the representative procedures described herein. Polypeptide variants preferably exhibit at least about 70%, more preferably at least about 90% and most preferably at least about 95% identity (determined as described below) to the identified polypeptides.

[0192] As used herein, a “conservative substitution” is one in which an amino acid is substituted for another amino acid that has similar properties, such that one skilled in the art of peptide chemistry would expect the secondary structure and hydropathic nature of the polypeptide to be substantially unchanged. In general, the following groups of amino acids represent conservative changes: (1) ala, pro, gly, glu, asp, gln, asn, ser, thr; (2) cys, ser, tyr, thr; (3) val, ile, leu, met, ala, phe; (4) lys, arg, his; and (5) phe, tyr, trp, his.

[0193] Variants may also, or alternatively, contain other modifications, including the deletion or addition of amino acids that have minimal influence on the antigenic properties, secondary structure and hydropathic nature of the polypeptide. For example, a polypeptide may be conjugated to a signal (or leader) sequence at the N-terminal end of the protein which co-translationally or post-translationally directs transfer of the protein. The polypeptide may also be conjugated to a linker or other sequence for ease of synthesis, purification or identification of the polypeptide (e.g., poly-His), or to enhance binding of the polypeptide to a solid support. For example, a polypeptide may be conjugated to an immunoglobulin Fc region.

[0194] A nucleotide “variant” is a sequence that differs from the recited nucleotide sequence in having one or more nucleotide deletions, substitutions or additions. Such modifications may be readily introduced using standard mutagenesis techniques, such as oligonucleotide-directed site-specific mutagenesis as taught, for example, by Adelman et al. (DNA, 2:183, 1983). Nucleotide variants may be naturally occurring allelic variants, or non-naturally occurring variants. Variant nucleotide sequences preferably exhibit at least about 70%, more preferably at least about 80% and most preferably at least about 90% identity (determined as described below) to the recited sequence.

[0195] The breast tumor antigens provided by the present invention include variants that are encoded by DNA sequences which are substantially homologous to one or more of the DNA sequences specifically recited herein. “Substantial homology,” as used herein, refers to DNA sequences that are capable of hybridizing under moderately stringent conditions. Suitable moderately stringent conditions include prewashing in a solution of 5×SSC, 0.5% SDS, 1.0 mM EDTA (pH 8.0); hybridizing at 50° C.-65° C., 5×SSC, overnight or, in the event of cross-species homology, at 45° C. with 0.5×SSC; followed by washing twice at 65° C. for 20 minutes with each of 2×, 0.5× and 0.2×SSC containing 0.1% SDS. Such hybridizing DNA sequences are also within the scope of this invention, as are nucleotide sequences that, due to code degeneracy, encode an immunogenic polypeptide that is encoded by a hybridizing DNA sequence.

[0196] Two nucleotide or polypeptide sequences are said to be “identical” if the sequence of nucleotides or amino acid residues in the two sequences is the same when aligned for maximum correspondence as described below. Comparisons between two sequences are typically performed by comparing the sequences over a comparison window to identify and compare local regions of sequence similarity. A “comparison window” as used herein, refers to a segment of at least about 20 contiguous positions, usually 30 to about 75, 40 to about 50, in which a sequence may be compared to a reference sequence of the same number of contiguous positions after the two sequences are optimally aligned.

[0197] Optimal alignment of sequences for comparison may be conducted using the Megalign program in the Lasergene suite of bioinformatics software (DNASTAR, Inc., Madison, Wis.), using default parameters. This program embodies several alignment schemes described in the following references: Dayhoff, M. O. (1978) A model of evolutionary change in proteins—Matrices for detecting distant relationships. In Dayhoff, M. O. (ed.) Atlas of Protein Sequence and Structure, National Biomedical Resarch Foundaiton, Washington D.C. Vol. 5, Suppl. 3, pp. 345-358; Hein J. (1990) Unified Approach to Alignment and Phylogenes pp. 626-645 Methods in Enzymology vol. 183, Academic Press, Inc., San Diego, Calif.; Higgins, D. G. and Sharp, P. M. (1989) Fast and sensitive multiple sequence alignments on a microcomputer CABIOS 5:151-153; Myers, E. W. and Muller W. (1988) Optimal alignments in linear space CABIOS 4:11-17; Robinson, E. D. (1971) Comb. Theor 11:105; Santou, N. Nes, M. (1987) The neighbor joining method. A new method for reconstructing phylogenetic trees Mol. Biol. Evol. 4:406-425; Sneath, P. H. A. and Sokal, R. R. (1973) Numerical Taxonomy—the Principles and Practice of Numerical Taxonomy, Freeman Press, San Francisco, Calif.; Wilbur, W. J. and Lipman, D. J. (1983) Rapid similarity searches of nucleic acid and protein data banks Proc. Natl. Acad., Sci. USA 80:726-730.

[0198] Preferably, the “percentage of sequence identity” is determined by comparing two optimally aligned sequences over a window of comparison of at least 20 positions, wherein the portion of the polynucleotide sequence in the comparison window may comprise additions or deletions (i.e. gaps) of 20 percent or less, usually 5 to 15 percent, or 10 to 12 percent, as compared to the reference sequences (which does not comprise additions or deletions) for optimal alignment of the two sequences. The percentage is calculated by determining the number of positions at which the identical nucleic acid bases or amino acid residue occurs in both sequences to yield the number of matched positions, dividing the number of matched positions by the total number of positions in the reference sequence (i.e. the window size) and multiplying the results by 100 to yield the percentage of sequence identity.

[0199] The breast tumor antigens of the present invention, and polynucleotides encoding such antigens, may be isolated from breast tumor tissue using any of a variety of methods well known in the art. DNA sequences corresponding to a gene (or a portion thereof) encoding one of the inventive breast tumor antigens may be isolated from a breast tumor cDNA library using a subtraction technique as described in detail below. Examples of such DNA sequences are provided in SEQ ID NO: 1-61, 63-175, 178 and 180. Partial DNA sequences thus obtained may be used to design oligonucleotide primers for the amplification of full-length DNA sequences in a polymerase chain reaction (PCR), using techniques well known in the art (see, for example, Mullis et al., Cold Spring Harbor Symp. Quant. Biol., 51:263, 1987; Erlich ed., PCR Technology, Stockton Press, NY, 1989). Once a DNA sequence encoding a polypeptide is obtained, any of the above modifications may be readily introduced using standard mutagenesis techniques, such as oligonucleotide-directed site-specific mutagenesis as taught, for example, by Adelman et al. (DNA, 2:183, 1983).

[0200] The breast tumor polypeptides disclosed herein may also be generated by synthetic or recombinant means. Synthetic polypeptides having fewer than about 100 amino acids, and generally fewer than about 50 amino acids, may be generated using techniques well known to those of ordinary skill in the art. For example, such polypeptides may be synthesized using any of the commercially available solid-phase techniques, such as the Merrifield solid-phase synthesis method, where amino acids are sequentially added to a growing amino acid chain (see, for example, Merrifield, J. Am. Chem. Soc. 85:2149-2146, 1963). Equipment for automated synthesis of polypeptides is commercially available from suppliers such as Perkin Elmer/Applied BioSystems Division (Foster City, Calif.), and may be operated according to the manufacturer's instructions.

[0201] Alternatively, any of the above polypeptides may be produced recombinantly by inserting a DNA sequence that encodes the polypeptide into an expression vector and expressing the protein in an appropriate host. Any of a variety of expression vectors known to those of ordinary skill in the art may be employed to express recombinant polypeptides of this invention. Expression may be achieved in any appropriate host cell that has been transformed or transfected with an expression vector containing a polynucleotide that encodes a recombinant polypeptide. Suitable host cells include prokaryotes, yeast and higher eukaryotic cells. Preferably, the host cells employed are E. coli, yeast or a mammalian cell line, such as CHO cells. The DNA sequences expressed in this manner may encode naturally occurring polypeptides, portions of naturally occurring polypeptides, or other variants thereof.

[0202] In general, regardless of the method of preparation, the polypeptides disclosed herein are prepared in an isolated, substantially pure, form (i.e., the polypeptides are homogenous as determined by amino acid composition and primary sequence analysis). Preferably, the polypeptides are at least about 90% pure, more preferably at least about 95% pure and most preferably at least about 99% pure. In certain preferred embodiments, described in more detail below, the substantially pure polypeptides are incorporated into pharmaceutical compositions or vaccines for use in one or more of the methods disclosed herein.

[0203] In a related aspect, the present invention provides fusion proteins comprising a first and a second inventive polypeptide or, alternatively, a polypeptide of the present invention and a known breast tumor antigen, together with variants of such fusion proteins.

[0204] A DNA sequence encoding a fusion protein of the present invention is constructed using known recombinant DNA techniques to assemble separate DNA sequences encoding the first and second polypeptides into an appropriate expression vector. The 3′ end of a DNA sequence encoding the first polypeptide is ligated, with or without a peptide linker, to the 5′ end of a DNA sequence encoding the second polypeptide so that the reading frames of the sequences are in phase to permit mRNA translation of the two DNA sequences into a single fusion protein that retains the biological activity of both the first and the second polypeptides.

[0205] A peptide linker sequence may be employed to separate the first and the second polypeptides by a distance sufficient to ensure that each polypeptide folds into its secondary and tertiary structures. Such a peptide linker sequence is incorporated into the fusion protein using standard techniques well known in the art. Suitable peptide linker sequences may be chosen based on the following factors: (1) their ability to adopt a flexible extended conformation; (2) their inability to adopt a secondary structure that could interact with functional epitopes on the first and second polypeptides; and (3) the lack of hydrophobic or charged residues that might react with the polypeptide functional epitopes. Preferred peptide linker sequences contain Gly, Asn and Ser residues. Other near neutral amino acids, such as Thr and Ala may also be used in the linker sequence. Amino acid sequences which may be usefully employed as linkers include those disclosed in Maratea et al., Gene 40:39-46, 1985; Murphy et al., Proc. Natl. Acad. Sci. USA 83:8258-8262, 1986; U.S. Pat. No. 4,935,233 and U.S. Pat. No. 4,751,180. The linker sequence may be from 1 to about 50 amino acids in length. Peptide sequences are not required when the first and second polypeptides have non-essential N-terminal amino acid regions that can be used to separate the functional domains and prevent steric interference.

[0206] The ligated DNA sequences are operably linked to suitable transcriptional or translational regulatory elements. The regulatory elements responsible for expression of DNA are located only 5′ to the DNA sequence encoding the first polypeptides. Similarly, stop codons require to end translation and transcription termination signals are only present 3′ to the DNA sequence encoding the second polypeptide.

[0207] Fusion proteins are also provided that comprise a polypeptide of the present invention together with an unrelated immunogenic protein. Preferably the immunogenic protein is capable of eliciting a recall response. Examples of such proteins include tetanus, tuberculosis and hepatitis proteins (see, for example, Stoute et al. New Engl. J. Med., 336:86-91 (1997)).

[0208] Polypeptides of the present invention that comprise an immunogenic portion of a breast tumor antigen may generally be used for immunotherapy of breast cancer, wherein the polypeptide stimulates the patient's own immune response to breast tumor cells. The present invention thus provides methods for using one or more of the immunoreactive polypeptides encoded by a polynucleotide comprising a sequence of SEQ ID NO: 1-61, 63-175, 178 and 180 (or fusion proteins comprising one or more such polypeptides and/or DNA encoding such polypeptides) for immunotherapy of breast cancer in a patient. As used herein, a “patient” refers to any warm-blooded animal, preferably a human. A patient may be afflicted with a disease, or may be free of detectable disease. Accordingly, the above immunoreactive polypeptides (or fusion proteins or polynucleotides encoding such polypeptides) may be used to treat breast cancer or to inhibit the development of breast cancer. The polypeptides may be administered either prior to or following surgical removal of primary tumors and/or treatment by administration of radiotherapy and conventional chemotherapeutic drugs.

[0209] In these aspects, the polypeptide or fusion protein is generally present within a pharmaceutical composition and/or a vaccine. Pharmaceutical compositions may comprise one or more polypeptides, each of which may contain one or more of the inventive sequences (or variants thereof), and a physiologically acceptable carrier. The vaccines may comprise one or more such polypeptides and a non-specific immune response enhancer, wherein the non-specific immune response enhancer is capable of eliciting or enhancing an immune response to an exogenous antigen. Examples of non-specific-immune response enhancers include adjuvants, biodegradable microspheres (e.g., polylactic galactide) and liposomes (into which the polypeptide is incorporated). Pharmaceutical compositions and vaccines may also contain other epitopes of breast tumor antigens, either incorporated into a combination polypeptide (i.e., a single polypeptide that contains multiple epitopes) or present within a separate polypeptide.

[0210] Alternatively, a pharmaceutical composition or vaccine may contain DNA encoding one or more of the above polypeptides, such that the polypeptide is generated in situ. In such pharmaceutical compositions and vaccines, the DNA may be present within any of a variety of delivery systems known to those of ordinary skill in the art, including nucleic acid expression systems, bacteria and viral expression systems. Appropriate nucleic acid expression systems contain the necessary DNA sequences for expression in the patient (such as a suitable promoter). Bacterial delivery systems involve the administration of a bacterium (such as Bacillus-Calmette-Gruerrin) that expresses an epitope of a breast tumor cell antigen on its cell surface. In a preferred embodiment, the DNA may be introduced using a viral expression system (e.g., vaccinia or other pox virus, retrovirus, or adenovirus), which may involve the use of a non-pathogenic (defective), replication competent virus. Suitable systems are disclosed, for example, in Fisher-Hoch et al., PNAS 86:317-321, 1989; Flexner et al., Ann. N.Y Acad. Sci. 569:86-103, 1989; Flexner et al., Vaccine 8:17-21, 1990; U.S. Pat. Nos. 4,603,112, 4,769,330, and 5,017,487; WO 89/01973; U.S. Pat. No. 4,777,127; GB 2,200,651; EP 0,345,242; WO 91/02805; Berkner, Biotechniques 6:616-627, 1988; Rosenfeld et al., Science 252:431-434, 1991; Kolls et al., PNAS 91:215-219, 1994; Kass-Eisler et al., PNAS 90:11498-11502, 1993; Guzman et al., Circulation 88:2838-2848, 1993; and Guzman et al., Cir. Res. 73:1202-1207, 1993. Techniques for incorporating DNA into such expression systems are well known to those of ordinary skill in the art. The DNA may also be “naked,” as described, for example, in published PCT application WO 90/11092, and Ulmer et al., Science 259:1745-1749, 1993, reviewed by Cohen, Science 259:1691-1692, 1993. The uptake of naked DNA may be increased by coating the DNA onto biodegradable beads, which are efficiently transported into the cells.

[0211] Routes and frequency of administration, as well as dosage, will vary from individual to individual and may parallel those currently being used in immunotherapy of other diseases. In general, the pharmaceutical compositions and vaccines may be administered by injection (e.g., intracutaneous, intramuscular, intravenous or subcutaneous), intranasally (e.g., by aspiration) or orally. Between 1 and 10 doses may be administered over a 3-24 week period. Preferably, 4 doses are administered, at an interval of 3 months, and booster administrations may be given periodically thereafter. Alternate protocols may be appropriate for individual patients. A suitable dose is an amount of polypeptide or DNA that is effective to raise an immune response (cellular and/or humoral) against breast tumor cells in a treated patient. A suitable immune response is at least 10-50% above the basal (ie., untreated) level. In general, the amount of polypeptide present in a dose (or produced in situ by the DNA in a dose) ranges from about 1 pg to about 100 mg per kg of host, typically from about 10 pg to about 1 mg, and preferably from about 100 pg to about 1 μg. Suitable dose sizes will vary with the size of the patient, but will typically range from about 0.01 mL to about 5 mL.

[0212] While any suitable carrier known to those of ordinary skill in the art may be employed in the pharmaceutical compositions of this invention, the type of carrier will vary depending on the mode of administration. For parenteral administration, such as subcutaneous injection, the carrier preferably comprises water, saline, alcohol, a lipid, a wax and/or a buffer. For oral administration, any of the above carriers or a solid carrier, such as mannitol, lactose, starch, magnesium stearate, sodium saccharine, talcum, cellulose, glucose, sucrose, and/or magnesium carbonate, may be employed. Biodegradable microspheres (e.g., polylactic glycolide) may also be employed as carriers for the pharmaceutical compositions of this invention. Suitable biodegradable microspheres are disclosed, for example, in U.S. Pat. Nos. 4,897,268 and 5,075,109.

[0213] Any of a variety of non-specific immune response enhancers may be employed in the vaccines of this invention. For example, an adjuvant may be included. Most adjuvants contain a substance designed to protect the antigen from rapid catabolism, such as aluminum hydroxide or mineral oil, and a nonspecific stimulator of immune response, such as lipid A, Bordella pertussis or Mycobacterium tuberculosis. Such adjuvants are commercially available as, for example, Freund's Incomplete Adjuvant and Complete Adjuvant (Difco Laboratories, Detroit, Mich.) and Merck Adjuvant 65 (Merck and Company, Inc., Rahway, N.J.).

[0214] Polypeptides disclosed herein may also be employed in adoptive immunotherapy for the treatment of cancer. Adoptive immunotherapy may be broadly classified into either active or passive immunotherapy. In active immunotherapy, treatment relies on the in vivo stimulation of the endogenous host immune system to react against tumors with the administration of immune response-modifying agents (for example, tumor vaccines, bacterial adjuvants, and/or cytokines).

[0215] In passive immunotherapy, treatment involves the delivery of biologic reagents with established tumor-immune reactivity (such as effector cells or antibodies) that can directly or indirectly mediate antitumor effects and does not necessarily depend on an intact host immune system. Examples of effector cells include T lymphocytes (for example, CD8+ cytotoxic T-lymphocyte, CD4+ T-helper, gamma/delta T lymphocytes, tumor-infiltrating lymphocytes), killer cells (such as Natural Killer cells, lymphokine-activated killer cells), B cells, or antigen presenting cells (such as dendritic cells and macrophages) expressing the disclosed antigens. The polypeptides disclosed herein may also be used to generate antibodies or anti-idiotypic antibodies (as in U.S. Pat. No. 4,918,164), for passive immunotherapy.

[0216] The predominant method of procuring adequate numbers of T-cells for adoptive immunotherapy is to grow immune T-cells in vitro. Culture conditions for expanding single antigen-specific T-cells to several billion in number with retention of antigen recognition in vivo are well known in the art. These in vitro culture conditions typically utilize intermittent stimulation with antigen, often in the presence of cytokines, such as IL-2, and non-dividing feeder cells. As noted above, the immunoreactive polypeptides described herein may be used to rapidly expand antigen-specific T cell cultures in order to generate sufficient number of cells for immunotherapy. In particular, antigen-presenting cells, such as dendritic, macrophage, monocyte, fibroblast or B-cells, may be pulsed with immunoreactive polypeptides or polynucleotide sequence(s) may be introduced into: antigen presenting cells, using standard techniques well known in the art. For example, antigen presenting cells may be transfected or transduced with a polynucleotide sequence, wherein said sequence contains a promoter region appropriate for inducing expression, and can be expressed as part of a recombinant virus or other expression system. Several viral vectors may be used to transduce an antigen presenting cell, including pox virus, vaccinia virus, and adenovirus. Antigen presenting cells may be transfected with polynucleotide sequences disclosed herein by a variety of means, including gene-gun technology, lipid-mediated delivery, electroporation, osmotic shock, and particulate delivery mechanisms, resulting in efficient and acceptable expression levels as determined by one of ordinary skill in the art. For cultured T-cells to be effective in therapy, the cultured T-cells must be able to grow and distribute widely and to survive long term in vivo. Studies have demonstrated that cultured T-cells can be induced to grow in vivo and to survive long term in substantial numbers by repeated stimulation with antigen supplemented with IL-2 (see, for example, Cheever et al. Ibid).

[0217] The polypeptides disclosed herein may also be employed to generate and/or isolate tumor-reactive T-cells, which can then be administered to the patient. In one technique, antigen-specific T-cell lines may be generated by in vivo immunization with short peptides corresponding to immunogenic portions of the disclosed polypeptides. The resulting antigen specific CD8+ CTL clones may be isolated from the patient, expanded using standard tissue culture techniques, and returned to the patient.

[0218] Alternatively, peptides corresponding to immunogenic portions of the polypeptides may be employed to generate tumor reactive T cell subsets by selective in vitro stimulation and expansion of autologous T cells to provide antigen-specific T cells which may be subsequently transferred to the patient as described, for example, by Chang et al. (Crit. Rev. Oncol. Hematol., 22(3), 213, 1996). Cells of the immune system, such as T cells, may be isolated from the peripheral blood of a patient, using a commercially available cell separation system. The separated cells are stimulated with one or more of the immunoreactive polypeptides contained within a delivery vehicle, such as a microsphere, to provide antigen-specific T cells. The population of tumor antigen-specific T cells is then expanded using standard techniques and the cells are administered back to the patient.

[0219] In other embodiments, T-cell and/or antibody receptors specific for the polypeptides disclosed herein can be cloned, expanded, and transferred into other vectors or effector cells for use in adoptive immunotherapy. In particular, T cells may be transfected with the appropriate genes to express the variable domains from tumor specific monoclonal antibodies as the extracellular recognition elements and joined to the T cell receptor signaling chains, resulting in T cell activation, specific lysis, and cytokine release. This enables the T cell to redirect its specificity in an MHC-independent manner. See for example, Eshhar, Z., Cancer Immunol Immunother, 45(3-4):131-6, 1997 and Hwu, P., et al, Cancer Res, 55(15):3369-73, 1995. Another embodiment may include the transfection of tumor antigen specific alpha and beta T cell receptor chains into alternate T cells, as in Cole, D J, et al, Cancer Res, 55(4):748-52, 1995.

[0220] In further embodiments, syngeneic or autologous dendritic cells may be pulsed with peptides corresponding to at least an immunogenic portion of a polypeptide disclosed herein. The resulting antigen-specific dendritic cells may either be transferred into a patient, or employed to stimulate T cells to provide antigen-specific T cells which may, in turn, be administered to a patient. The use of peptide-pulsed dendritic cells to generate antigen-specific T cells and the subsequent use of such antigen-specific T cells to eradicate tumors in a murine model has been demonstrated by Cheever et al. (“Therapy With Cultured T Cells: Principles Revisited,” Immunological Reviews, 157:177, 1997). Additionally vectors expressing the disclosed polynucleotides may be introduced into stem cells taken from the patient and clonally propagated in vitro for autologous transplant back into the same patient.

[0221] In one specific embodiment, cells of the immune system, such as T cells, may be isolated from the peripheral blood of a patient, using a commercially available cell separation system, such as CellPro Incorporated's (Bothell, Wash.) CEPRATE™ system (see U.S. Pat. No. 5,240,856; U.S. Pat. No. 5,215,926; WO 89/06280; WO 91/16116 and WO 92/07243). The separated cells are stimulated with one or more of the immunoreactive polypeptides contained within a delivery vehicle, such as a microsphere, to provide antigen-specific T cells. The population of tumor antigen-specific T cells is then expanded using standard techniques and the cells are administered back to the patient.

[0222] Additionally vectors expressing the disclosed polynucleotides may be introduced into stem cells taken from the patient and clonally propagated in vitro for autologous transplant back into the same patient.

[0223] Polypeptides of the present invention may also, or alternatively, be used to generate binding agents, such as antibodies or fragments thereof, that are capable of detecting metastatic human breast tumors. Binding agents of the present invention may generally be prepared using methods known to those of ordinary skill in the art, including the representative procedures described herein. Binding agents are capable of differentiating between patients with and without breast cancer, using the representative assays described herein. In other words, antibodies or other binding agents raised against a breast tumor antigen, or a suitable portion thereof, will generate a signal indicating the presence of primary or metastatic breast cancer in at least about 20% of patients afflicted with the disease, and will generate a negative signal indicating the absence of the disease in at least about 90% of individuals without primary or metastatic breast cancer. Suitable portions of such breast tumor antigens are portions that are able to generate a binding agent that indicates the presence of primary or metastatic breast cancer in substantially all (i.e., at least about 80%, and preferably at least about 90%) of the patients for which breast cancer would be indicated using the full length antigen, and that indicate the absence of breast cancer in substantially all of those samples that would be negative when tested with full length antigen. The representative assays described below, such as the two-antibody sandwich assay, may generally be employed for evaluating the ability of a binding agent to detect metastatic human breast tumors.

[0224] The ability of a polypeptide prepared as described herein to generate antibodies capable of detecting primary or metastatic human breast tumors may generally be evaluated by raising one or more antibodies against the polypeptide (using, for example, a representative method described herein) and determining the ability of such antibodies to detect such tumors in patients. This determination may be made by assaying biological samples from patients with and without primary or metastatic breast cancer for the presence of a polypeptide that binds to the generated antibodies. Such test assays may be performed, for example, using a representative procedure described below. Polypeptides that generate antibodies capable of detecting at least 20% of primary or metastatic breast tumors by such procedures are considered to be useful in assays for detecting primary or metastatic human breast tumors Polypeptide specific antibodies may be used alone or in combination to improve sensitivity.

[0225] Polypeptides capable of detecting primary or metastatic human breast tumors may be used as markers for diagnosing breast cancer or for monitoring disease progression in patients. In one embodiment, breast cancer in a patient may be diagnosed by evaluating a biological sample obtained from the patient for the level of one or more of the above polypeptides, relative to a predetermined cut-off value. As used herein, suitable “biological samples” include blood, sera and urine.

[0226] The level of one or more of the above polypeptides may be evaluated using any binding agent specific for the polypeptide(s). A “binding agent,” in the context of this invention, is any agent (such as a compound or a cell) that binds to a polypeptide as described above. As used herein, “binding” refers to a noncovalent association between two separate molecules (each of which may be free (ie., in solution) or present on the surface of a cell or a solid support), such that a “complex” is formed. Such a complex may be free or immobilized (either covalently or noncovalently) on a support material. The ability to bind may generally be evaluated by determining a binding constant for the formation of the complex. The binding constant is the value obtained when the concentration of the complex is divided by the product of the component concentrations. In general, two compounds are said to “bind” in the context of the present invention when the binding constant for complex formation exceeds about 10³ L/mol. The binding constant may be determined using methods well known to those of ordinary skill in the art.

[0227] Any agent that satisfies the above requirements may be a binding agent. For example, a binding agent may be a ribosome with or without a peptide component, an RNA molecule or a peptide. In a preferred embodiment, the binding partner is an antibody, or a fragment thereof. Such antibodies may be polyclonal, or monoclonal. In addition, the antibodies may be single chain, chimeric, CDR-grafted or humanized. Antibodies may be prepared by the methods described herein and by other methods well known to those of skill in the art.

[0228] There are a variety of assay formats known to those of ordinary skill in the art for using a binding partner to detect polypeptide markers in a sample. See, e.g., Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, 1988. In a preferred embodiment, the assay involves the use of binding partner immobilized on a solid support to bind to and remove the polypeptide from the remainder of the sample. The bound polypeptide may then be detected using a second binding partner that contains a reporter group. Suitable second binding partners include antibodies that bind to the binding partner/polypeptide complex. Alternatively, a competitive assay may be utilized, in which a polypeptide is labeled with a reporter group and allowed to bind to the immobilized binding partner after incubation of the binding partner with the sample. The extent to which components of the sample inhibit the binding of the labeled polypeptide to the binding partner is indicative of the reactivity of the sample with the immobilized binding partner.

[0229] The solid support may be any material known to those of ordinary skill in the art to which the antigen may be attached. For example, the solid support may be a test well in a microtiter plate or a nitrocellulose or other suitable membrane. Alternatively, the support may be a bead or disc, such as glass, fiberglass, latex or a plastic material such as polystyrene or polyvinylchloride. The support may also be a magnetic particle or a fiber optic sensor, such as those disclosed, for example, in U.S. Pat. No. 5,359,681. The binding agent may be immobilized on the solid support using a variety of techniques known to those of skill in the art, which are amply described in the patent and scientific literature. In the context of the present invention, the term “immobilization” refers to both noncovalent association, such as adsorption, and covalent attachment (which may be a direct linkage between the antigen and functional groups on the support or may be a linkage by way of a cross-linking agent). Immobilization by adsorption to a well in a microtiter plate or to a membrane is preferred. In such cases, adsorption may be achieved by contacting the binding agent, in a suitable buffer, with the solid support for a suitable amount of time. The contact time varies with temperature, but is typically between about 1 hour and about 1 day. In general, contacting a well of a plastic microtiter plate (such as polystyrene or polyvinylchloride) with an amount of binding agent ranging from about 10 ng to about 10 μg, and preferably about 100 ng to about 1 μg,; is sufficient to immobilize an adequate amount of binding agent.

[0230] Covalent attachment of binding agent to a solid support may generally be achieved by first reacting the support with a bifunctional reagent that will react with both the support and a functional group, such as a hydroxyl or amino group, on the binding agent. For example, the binding agent may be covalently attached to supports having an appropriate polymer coating using benzoquinone or by condensation of an aldehyde group on the support with an amine and an active hydrogen on the binding partner (see, e.g., Pierce Immunotechnology Catalog and Handbook, 1991, at A12-A13).

[0231] In certain embodiments, the assay is a two-antibody sandwich assay. This assay may be performed by first contacting an antibody that has been immobilized on a solid support, commonly the well of a microtiter plate, with the sample, such that polypeptides within the sample are allowed to bind to the immobilized antibody. Unbound sample is then removed from the immobilized polypeptide-antibody complexes and a second antibody (containing a reporter group) capable of binding to a different site on the polypeptide is added. The amount of second antibody that remains bound to the solid support is then determined using a method appropriate for the specific reporter group.

[0232] More specifically, once the antibody is immobilized on the support as described above, the remaining protein binding sites on the support are typically blocked. Any suitable blocking agent known to those of ordinary skill in the art, such as bovine serum albumin or Tween 20™ (Sigma Chemical Co., St. Louis, Mo.). The immobilized antibody is then incubated with the sample, and polypeptide is allowed to bind to the antibody. The sample may be diluted with a suitable diluent, such as phosphate-buffered saline (PBS) prior to incubation. In general, an appropriate contact time (i.e., incubation time) is that period of time that is sufficient to detect the presence of polypeptide within a sample obtained from an individual with breast cancer. Preferably, the contact time is sufficient to achieve a level of binding that is at least about 95% of that achieved at equilibrium between bound and unbound polypeptide. Those of ordinary skill in the art will recognize that the time necessary to achieve equilibrium may be readily determined by assaying the level of binding that occurs over a period of time. At room temperature, an incubation time of about 30 minutes is generally sufficient.

[0233] Unbound sample may then be removed by washing the solid support with an appropriate buffer, such as PBS containing 0.1% Tween 20™. The second antibody, which contains a reporter group, may then be added to the solid support. Preferred reporter groups include enzymes (such as horseradish peroxidase), substrates, cofactors, inhibitors, dyes, radionuclides, luminescent groups, fluorescent groups and biotin. The conjugation of antibody to reporter group may be achieved using standard methods known to those of ordinary skill in the art.

[0234] The second antibody is then incubated with the immobilized antibody-polypeptide complex for an amount of time sufficient to detect the bound polypeptide. An appropriate amount of time may generally be determined by assaying the level of binding that occurs over a period of time. Unbound second antibody is then removed and bound second antibody is detected using the reporter group. The method employed for detecting the reporter group depends upon the nature of the reporter group. For radioactive groups, scintillation counting or autoradiographic methods are generally appropriate. Spectroscopic methods may be used to detect dyes, luminescent groups and fluorescent groups. Biotin may be detected using avidin, coupled to a different reporter group (commonly a radioactive or fluorescent group or an enzyme). Enzyme reporter groups may generally be detected by the addition of substrate (generally for a specific period of time), followed by spectroscopic or other analysis of the reaction products.

[0235] To determine the presence or absence of breast cancer, the signal detected from the reporter group that remains bound to the solid support is generally compared to a signal that corresponds to a predetermined cut-off value. In one preferred embodiment, the cut-off value is the average mean signal obtained when the immobilized antibody is incubated with samples from patients without breast cancer. In general, a sample generating a signal that is three standard deviations above the predetermined cut-off value is considered positive for breast cancer. In an alternate preferred embodiment, the cut-off value is determined using a Receiver Operator Curve, according to the method of Sackett et al., Clinical Epidemiology: A Basic Science for Clinical Medicine, Little Brown and Co., 1985, p. 106-7. Briefly, in this embodiment, the cut-off value may be determined from a plot of pairs of true positive rates (i.e., sensitivity) and false positive rates (100%-specificity) that correspond to each possible cut-off value for the diagnostic test result. The cut-off value on the plot that is the closest to the upper left-hand corner (i.e., the value that encloses the largest area) is the most accurate cut-off value, and a sample generating a signal that is higher than the cut-off value determined by this method may be considered positive. Alternatively, the cut-off value may be shifted to the left along the plot, to minimize the false positive rate, or to the right, to minimize the false negative rate. In general, a sample generating a signal that is higher than the cut-off value determined by this method is considered positive for breast cancer.

[0236] In a related embodiment, the assay is performed in a flow-through or strip test format, wherein the antibody is immobilized on a membrane, such as nitrocellulose. In the flow-through test, polypeptides within the sample bind to the immobilized antibody as the sample passes through the membrane. A second, labeled antibody then binds to the antibody-polypeptide complex as a solution containing the second antibody flows through the membrane. The detection of bound second antibody may then be performed as described above. In the strip test format, one end of the membrane to which antibody is bound is immersed in a solution containing the sample. The sample migrates along the membrane through a region containing second antibody and to the area of immobilized antibody. Concentration of second antibody at the area of immobilized antibody indicates the presence of breast cancer. Typically, the concentration of second antibody at that site generates a pattern, such as a line, that can be read visually. The absence of such a pattern indicates a negative result. In general, the amount of antibody immobilized on the membrane is selected to generate a visually discernible pattern when the biological sample contains a level of polypeptide that would be sufficient to generate a positive signal in the two-antibody sandwich assay, in the format discussed above. Preferably, the amount of antibody immobilized on the membrane ranges from about 25 ng to about 1 μg, and more preferably from about 50 ng to about 500 ng. Such tests can typically be performed with a very small amount of biological sample.

[0237] Of course, numerous other assay protocols exist that are suitable for use with the antigens or antibodies of the present invention. The above descriptions are intended to be exemplary only.

[0238] In another embodiment, the above polypeptides may be used as markers for the progression of breast cancer. In this embodiment, assays as described above for the diagnosis of breast cancer may be performed over time, and the change in the level of reactive polypeptide(s) evaluated. For example, the assays may be performed every 24-72 hours for a period of 6 months to 1 year, and thereafter performed as needed. In general, breast cancer is progressing in those patients in whom the level of polypeptide detected by the binding agent increases over time. In contrast, breast cancer is not progressing when the level of reactive polypeptide either remains constant or decreases with time.

[0239] Antibodies for use in the above methods may be prepared by any of a variety of techniques known to those of ordinary skill in the art. See, e.g., Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, 1988. In one such technique, an immunogen comprising the antigenic polypeptide is initially injected into any of a wide variety of mammals (e.g., mice, rats, rabbits; sheep and goats). In this step, the polypeptides of this invention may serve as the immunogen without modification. Alternatively, particularly for relatively short polypeptides, a superior immune response may be elicited if the polypeptide is joined to a carrier protein, such as bovine serum albumin or keyhole limpet hemocyanin. The immunogen is injected into the animal host, preferably according to a predetermined schedule incorporating one or more booster immunizations, and the animals are bled periodically. Polyclonal antibodies specific for the polypeptide may then be purified from such antisera by, for example, affinity chromatography using the polypeptide coupled to a suitable solid support.

[0240] Monoclonal antibodies specific for the antigenic polypeptide of interest may be prepared, for example, using the technique of Kohler and Milstein, Eur. J. Immunol. 6:511-519, 1976, and improvements thereto. Briefly, these methods involve the preparation of immortal cell lines capable of producing antibodies having the desired specificity (i.e., reactivity with the polypeptide of interest). Such cell lines may be produced, for example, from spleen cells obtained from an animal immunized as described above. The spleen cells are then immortalized by, for example, fusion with a myeloma cell fusion partner, preferably one that is syngeneic with the immunized animal. A variety of fusion techniques may be employed. For example, the spleen cells and myeloma cells may be combined with a nonionic detergent for a few minutes and then plated at low density on a selective medium that supports the growth of hybrid cells, but not myeloma cells. A preferred selection technique uses HAT (hypoxanthine, aminopterin, thymidine) selection. After a sufficient time, usually about 1 to 2 weeks, colonies of hybrids are observed. Single colonies are selected and tested for binding activity against the polypeptide. Hybridomas having high reactivity and specificity are preferred.

[0241] Monoclonal antibodies may be isolated from the supernatants of growing hybridoma colonies. In addition, various techniques may be employed to enhance the yield, such as injection of the hybridoma cell line into the peritoneal cavity of a suitable vertebrate host, such as a mouse. Monoclonal antibodies may then be harvested from the ascites fluid or the blood. Contaminants may be removed from the antibodies by conventional techniques, such as chromatography, gel filtration, precipitation, and extraction. The polypeptides of this invention may be used in the purification process in, for example, an affinity chromatography step.

[0242] Monoclonal antibodies of the present invention may also be used as therapeutic reagents, to diminish or eliminate breast tumors. The antibodies may be used on their own (for instance, to inhibit metastases) or coupled to one or more therapeutic agents. Suitable agents in this regard include radionuclides, differentiation inducers, drugs, toxins, and derivatives thereof. Preferred radionuclides include ⁹⁰Y, ¹²³I, ¹²⁵I, ¹³¹I, ¹⁸⁶Re, ¹⁸⁸Re, ²¹¹At, and ²¹²Bi. Preferred drugs include methotrexate, and pyrimidine and purine analogs. Preferred differentiation inducers include phorbol esters and butyric acid. Preferred toxins include ricin, abrin, diptheria toxin, cholera toxin, gelonin, Pseudomonas exotoxin, Shigella toxin, and pokeweed antiviral protein.

[0243] A therapeutic agent may be coupled (e.g., covalently bonded) to a suitable monoclonal antibody either directly or indirectly (e.g., via a linker group). A direct reaction between an agent and an antibody is possible when each possesses a substituent capable of reacting with the other. For example, a nucleophilic group, such as an amino or sulfhydryl group, on one may be capable of reacting with a carbonyl-containing group, such as an anhydride or an acid halide, or with an alkyl group containing a good leaving group (e.g., a halide) on the other.

[0244] Alternatively, it may be desirable to couple a therapeutic agent and an antibody via a linker group. A linker group can function as a spacer to distance an antibody from an agent in order to avoid interference with binding capabilities. A linker group can also serve to increase the chemical reactivity of a substituent on an agent or an antibody, and thus increase the coupling efficiency. An increase in chemical reactivity may also facilitate the use of agents, or functional groups on agents, which otherwise would not be possible.

[0245] It will be evident to those skilled in the art that a variety of bifunctional or polyfunctional reagents, both homo- and hetero-functional (such as those described in the catalog of the Pierce Chemical Co., Rockford, Ill.), may be employed as the linker group. Coupling may be effected, for example, through amino groups, carboxyl groups, sulfhydryl groups or oxidized carbohydrate residues. There are numerous references describing such methodology, e.g., U.S. Pat. No. 4,671,958, to Rodwell et al.

[0246] Where a therapeutic agent is more potent when free from the antibody portion of the immunoconjugates of the present invention, it may be desirable to use a linker group which is cleavable during or upon internalization into a cell. A number of different cleavable linker groups have been described. The mechanisms for the intracellular release of an agent from these linker groups include cleavage by reduction of a disulfide bond (e.g., U.S. Pat. No. 4,489,710, to Spitler), by irradiation of a photolabile bond (e.g., U.S. Pat. No. 4,625,014, to Senter et al.), by hydrolysis of derivatized amino acid side chains (e.g., U.S. Pat. No. 4,638,045, to Kohn et al.), by serum complement-mediated hydrolysis (e.g., U.S. Pat. No. 4,671,958, to Rodwell et al.), and acid-catalyzed hydrolysis (e.g., U.S. Pat. No. 4,569,789, to Blattler et al.).

[0247] It may be desirable to couple more than one agent to an antibody. In one embodiment, multiple molecules of an agent are coupled to one antibody molecule. In another embodiment, more than one type of agent may be coupled to one antibody. Regardless of the particular embodiment, immunoconjugates with more than one agent may be prepared in a variety of ways. For example, more than one agent may be coupled directly to an antibody molecule, or linkers which provide multiple sites for attachment can be used. Alternatively, a carrier can be used.

[0248] A carrier may bear the agents in a variety of ways, including covalent bonding either directly or via a linker group. Suitable carriers include proteins such as albumins (e.g., U.S. Pat. No. 4,507,234, to Kato et al.), peptides and polysaccharides such as aminodextran (e.g., U.S. Pat. No. 4,699,784, to Shih et al.). A carrier may also bear an agent by noncovalent bonding or by encapsulation, such as within a liposome vesicle (e.g., U.S. Pat. Nos. 4,429,008 and 4,873,088). Carriers specific for radionuclide agents include radiohalogenated small molecules and chelating compounds. For example, U.S. Pat. No. 4,735,792 discloses representative radiohalogenated small molecules and their synthesis. A radionuclide chelate may be formed from chelating compounds that include those containing nitrogen and sulfur atoms as the donor atoms for binding the metal, or metal oxide, radionuclide. For example, U.S. Pat. No. 4,673,562, to Davison et al. discloses representative chelating compounds and their synthesis.

[0249] A variety of routes of administration for the antibodies and immunoconjugates may be used. Typically, administration will be intravenous, intramuscular, subcutaneous or in the bed of a resected tumor. It will be evident that the precise dose of the antibody/immunoconjugate will vary depending upon the antibody used, the antigen density on the tumor, and the rate of clearance of the antibody.

[0250] Diagnostic reagents of the present invention may also comprise DNA sequences encoding one or more of the above polypeptides, or one or more portions thereof. For example, at least two oligonucleotide primers may be employed in a polymerase chain reaction (PCR) based assay to amplify breast tumor-specific cDNA derived from a biological sample, wherein at least one of the oligonucleotide primers is specific for a polynucleotide encoding a breast tumor protein of the present invention. The presence of the amplified cDNA is then detected using techniques well known in the art, such as gel electrophoresis. Similarly, oligonucleotide probes specific for a polynucleotide encoding a breast tumor protein of the present invention may be used in a hybridization assay to detect the presence of an inventive polypeptide in a biological sample.

[0251] As used herein, the term “oligonucleotide primer/probe specific for a polynucleotide” means an oligonucleotide sequence that has at least about 60%, preferably at least about 75% and more preferably at least about 90%, identity to the polynucleotide in question. Oligonucleotide primers and/or probes which may be usefully employed in the inventive diagnostic methods preferably have at least about 10-40 nucleotides. In a preferred embodiment, the oligonucleotide primers comprise at least about 10 contiguous nucleotides of a polynucleotide comprising a sequence selected from SEQ ID NO: 1-61, 63-175, 178 and 180. Preferably, oligonucleotide probes for use in the inventive diagnostic methods comprise at least about 15 contiguous oligonucleotides of a polynucleotide comprising a sequence provided in SEQ ID NO: 1-61, 63-175, 178 and 180. Techniques for both PCR based assays and hybridization assays are well known in the art (see, for example, Mullis et al. Ibid; Ehrlich, Ibid). Primers or probes may thus be used to detect breast tumor-specific sequences in biological samples, including blood, urine and/or breast tumor tissue.

[0252] The following Examples are offered by way of illustration and not by way of limitation.

EXAMPLES Example 1

[0253] Isolation and Characterization of Breast Tumor Polypeptides

[0254] This Example describes the isolation of breast tumor polypeptides from a breast tumor cDNA library.

[0255] A cDNA subtraction library containing cDNA from breast tumor subtracted with normal breast cDNA was constructed as follows. Total RNA was extracted from primary tissues using Trizol reagent (Gibco BRL Life Technologies, Gaithersburg, Md.) as described by the manufacturer. The polyA+RNA was purified using an oligo(dT) cellulose column according to standard protocols. First strand cDNA was synthesized using the primer supplied in a Clontech PCR-Select cDNA Subtraction Kit (Clontech, Palo Alto, Calif.). The driver DNA consisted of cDNAs from two normal breast tissues with the tester cDNA being from three primary breast tumors. Double-stranded cDNA was synthesized for both tester and driver, and digested with a combination of endonucleases (MluI, MscI, PvuII, SalI and StuI) which recognize six base pairs DNA. This modification increased the average cDNA size dramatically compared with cDNAs generated according to Clontech's protocol. The digested tester cDNAs were ligated to two different adaptors and the subtraction was performed according to Clontech's protocol. The subtracted cDNAs were subjected to two rounds of PCR amplification, following the manufacturer's protocol. The resulting PCR products were subcloned into the TA cloning vector, pCRII (Invitrogen, San Diego, Calif.) and transformed into ElectroMax E. coli DH10B cells (Gibco BRL Life, Technologies) by electroporation. DNA was isolated from independent clones and sequenced using a Perkin Elmer/Applied Biosystems Division (Foster City, Calif.) Automated Sequencer Model 373A.

[0256] Sixty-three distinct cDNA clones were found in the subtracted breast tumor-specific cDNA library. The determined one strand (5′ or 3′) cDNA sequences for the clones are provided in SEQ ID NO: 1-61, 72 and 73, respectively. Comparison of these cDNA sequences with known sequences in the gene bank using the EMBL and GenBank databases (Release 97) revealed no significant homologies to the sequences provided in SEQ ID NO: 14, 21, 22, 27, 29, 30, 32, 38, 44, 45, 53, 72 and 73. The sequences of SEQ ID NO: 1, 3, 16, 17, 34, 48, 57, 60 and 61 were found to represent known human genes. The sequences of SEQ ID NO: 2, 4, 23, 39 and 50 were found to show some similarity to previously identified non-human genes. The remaining clones (SEQ ID NO: 5-13, 15, 18-20, 24-26, 28, 31, 33, 35-37, 40-43, 46, 47, 49, 51, 52, 54-56, 58 and 59) were found to show at least some degree of homology to previously identified expressed sequence tags (ESTs).

[0257] To determine mRNA expression levels of the isolated cDNA clones, cDNA clones from the breast subtraction described above were randomly picked and colony PCR amplified. Their mRNA expression levels in breast tumor, normal breast and various other normal tissues were determined using microarray technology (Synteni, Palo Alto, Calif.). Briefly, the PCR amplification products were arrayed onto slides in an array format, with each product occupying a unique location in the array. mRNA was extracted from the tissue sample to be tested, reverse transcribed, and fluorescent-labeled cDNA probes were generated. The microarrays were probed with the labeled cDNA probes, the slides scanned and fluorescence intensity was measured. Data was analyzed using Synteni provided GEMTOOLS Software. Of the seventeen cDNA clones examined, those of SEQ ID NO: 40, 46, 59 and 73 were found to be over-expressed in breast tumor and expressed at low levels in all normal tissues tested (breast, PBMC, colon, fetal tissue, salivary gland, bone marrow, lung, pancreas, large intestine, spinal cord, adrenal gland, kidney, pancreas, liver, stomach, skeletal muscle, heart, small intestine, skin, brain and human mammary epithelial cells). The clones of SEQ ID NO: 41 and 48 were found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested, with the exception of bone marrow. The clone of SEQ ID NO: 42 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested except bone marrow and spinal cord. The clone of SEQ ID NO: 43 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of spinal cord, heart and small intestine The clone of SEQ ID NO: 51 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of large intestine. The clone of SEQ ID NO: 54 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of PBMC, stomach and small intestine. The clone of SEQ ID NO: 56 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of large and small intestine, human mammary epithelia cells and SCID mouse-passaged breast tumor. The clone of SEQ ID NO: 60 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of spinal cord and heart. The clone of SEQ ID NO: 61 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of small intestine. The clone of SEQ ID NO: 72 was found to be over-expressed in breast tumor and expressed at low levels in all other tissues tested with the exception of colon and salivary gland.

[0258] The results of a Northern blot analysis of the clone SYN18C6 (SEQ ID NO: 40) are shown in FIG. 1. A predicted protein sequence encoded by SYN18C6 is provided in SEQ ID NO: 62.

[0259] Additional cDNA clones that are over-expressed in breast tumor tissue were isolated from breast cDNA subtraction libraries as follows. Breast subtraction libraries were prepared, as described above, by PCR-based subtraction employing pools of breast tumor cDNA as the tester and pools of either normal breast cDNA or cDNA from other normal tissues as the driver. cDNA clones from breast subtraction were randomly picked and colony PCR amplified and their mRNA expression levels in breast tumor, normal breast and various other normal tissues were determined using the microarray technology described above. Twenty-four distinct cDNA clones were found to be over-expressed in breast tumor and expressed at low levels in all normal tissues tested (breast, brain, liver, pancreas, lung, salivary gland, stomach, colon, kidney, bone marrow, skeletal muscle, PBMC, heart, small intestine, adrenal gland, spinal cord, large intestine and skin). The determined partial cDNA sequences for these clones are provided in SEQ ID NO: 63-87. Comparison of the sequences of SEQ ID NO: 74-87 with those in the gene bank as described above, revealed homology to previously identified human genes. No significant homologies were found to the sequences of SEQ ID NO: 63-73.

[0260] Three DNA isoforms for the clone B726P (partial sequence provided in SEQ ID NO: 71) were isolated as follows. A radioactive probe was synthesized from B726P by excising B726P DNA from a pT7Blue vector (Novagen) by a BamHI/XbaI restriction digest and using the resulting DNA as the template in a single-stranded PCR in the presence of [α-32P]dCTP. The sequence of the primer employed for this PCR is provided in SEQ ID NO: 177. The resulting radioactive probe was used to probe a directional cDNA library and a random-primed cDNA library made using RNA isolated from breast tumors. Eighty-five clones were identified, excised, purified and sequenced. Of these 85 clones, three were found to each contain a significant open reading frame. The determined cDNA sequence of the isoform B726P-20 is provided in SEQ ID NO: 175, with the corresponding predicted amino acid sequence being provided in SEQ ID NO: 176. The determined cDNA sequence of the isoform B726P-74 is provided in SEQ ID NO: 178, with the corresponding predicted amino acid sequence being provided in SEQ ID NO: 179. The determined cDNA sequence of the isoform B726P-79 is provided in SEQ ID NO: 180, with the corresponding predicted amino acid sequence being provided in SEQ ID NO: 181.

Example 2

[0261] Isolation and Characterization of Breast Tumor Polypeptides Obtained by PCR-Based Subtraction Using SCID-Passaged Tumor RNA

[0262] Human breast tumor antigens were obtained by PCR-based subtraction using SCID mouse passaged breast tumor RNA as follows. Human breast tumor was implanted in SCID mice and harvested on the first or sixth serial passage, as described in patent application Ser. No. 08/556,659 filed Nov. 13, 1995, U.S. Pat. No. ______. Genes found to be differentially expressed between early and late passage SCID tumor may be stage specific and therefore useful in therapeutic and diagnostic applications. Total RNA was prepared from snap frozen SCID passaged human breast tumor from both the first and sixth passage.

[0263] PCR-based subtraction was performed essentially as described above. In the first subtraction (referred to as T9), RNA from first passage tumor was subtracted from sixth passage tumor RNA to identify more aggressive, later passage-specific antigens. Of the 64 clones isolated and sequenced from this subtraction, no significant homologies were found to 30 of these clones, hereinafter referred to as: 13053, 13057, 13059, 13065, 13067, 13068, 13071-13073, 13075, 13078, 13079, 13081, 13082, 13092, 13097, 13101, 13102, 13131, 13133, 13119, 13135, 13139, 13140, 13146-13149, and 13151, with the exception of some previously identified expressed sequence tags (ESTs). The determined cDNA sequences for these clones are provided in SEQ ID NO: 88-116, respectively. The isolated cDNA sequences of SEQ ID NO: 117-140 showed homology to known genes.

[0264] In a second PCR-based subtraction, RNA from sixth passage tumor was subtracted from first passage tumor RNA to identify antigens down-regulated over multiple passages. Of the 36 clones isolated and sequenced, no significant homologies were found to nineteen of these clones, hereinafter referred to as: 14376, 14377, 14383, 14384, 14387, 14392, 14394, 14398, 14401, 14402, 14405, 14409, 14412, 14414-14416, 14419, 14426, and 14427, with the exception of some previously identified expressed sequence tags (ESTs). The determined cDNA sequences for these clones are provided in SEQ ID NO: 141-159, respectively. The isolated cDNA sequences of SEQ ID NO: 160-174 were found to show homology to previously known genes.

Example 3

[0265] Synthesis of Polypeptides

[0266] Polypeptides may be synthesized on an Perkin Elmer/Applied Biosystems Division 430A peptide synthesizer using FMOC chemistry with HPTU (O-Benzotriazole-N,N,N′,N′-tetramethyluronium hexafluorophosphate) activation. A Gly-Cys-Gly sequence may be attached to the amino terminus of the peptide to provide a method of conjugation, binding to an immobilized surface, or labeling of the peptide. Cleavage of the peptides from the solid support may be carried out using the following cleavage mixture: trifluoroacetic acid:ethanedithiol:thioanisole:water:phenol (40:1:2:2:3). After cleaving for 2 hours, the peptides may be precipitated in cold methyl-t-butyl-ether. The peptide pellets may then be dissolved in water containing 0.1% trifluoroacetic acid (TFA) and lyophilized prior to purification by C18 reverse phase HPLC. A gradient of 0%-60% acetonitrile (containing 0.1% TFA) in water (containing 0.1% TFA) may be used to elute the peptides. Following lyophilization of the pure fractions, the peptides may be characterized using electrospray or other types of mass spectrometry and by amino acid analysis.

[0267] From the foregoing, it will be appreciated that, although specific embodiments of the invention have been described herein for the purposes of illustration, various modifications may be made without deviating from the spirit and scope of the invention.

1 181 1 281 DNA Homo sapien 1 caatgacagt caatctctat cgacagcctg cttcatattt agctattgtt cgtattgcct 60 tctgtcctag gaacagtcat atctcaagtt caaatgccac aacctgagaa gcggtgggct 120 aagataggtc ctactgcaaa ccacccctcc atatttccgt acgcaattac aattcagttt 180 ctgtgacatc tctttacacc actggaggaa aaatgagata ttctctgatt tattctacta 240 taacactcta catagagcta tggtgagtgc taaccacatc g 281 2 300 DNA Homo sapien 2 gaggtcctgg gctaacctaa tggtttatta ttggtggaga gaaagatctg gaaatacttg 60 aggttattac atactagatt agcttctaat gtgaaccatt tttcttttaa cagtgataaa 120 ttattatttc cgaagttaac tgttcccttg gtcgtgatac acactcgatt aacaaacata 180 ctgttgtatt ttttccagtt ttgtttggct atgccaccac agtcatcccc agggtctata 240 catactatgt ctcaactgta ttatttgcca tttttggcat tagaatgctt cgggaaggct 300 3 302 DNA Homo sapien 3 ggccgaggta attggttaag tctaaagaga ttattattcc ttgatgtttg ctttgtattg 60 gctacaaatg tgcagaggta atacatatgt gatgtcgatg tctctgtctt tttttttgtc 120 tttaaaaaat aattggcagc aactgtattt gaataaaatg atttcttagt atgattgtac 180 agtaatgaat gaaagtggaa catgtttctt tttgaaaggg agagaattga ccatttattg 240 ttgtgatgtt taagttataa cttatcgagc acttttagta gtgataactg tttttaaact 300 tg 302 4 293 DNA Homo sapien 4 tgtaccaatc ctttggcaca agaatatgta agaactatag ttgtttttat tggtttttgt 60 tcttgagatt gttttcattc tgtttttgac tgtatctctt taggaggctg aggatggcat 120 tattgcttat gatgactgtg gggtgaaact gactattgct tttcaagcca aggatgtgga 180 aggatctact tctcctcaaa tacgagataa ggcaagataa ttctgctcat tcgagagagg 240 gttaagagtt gtcatcttaa tcataaatcc tgcaggatgg gttcttcaaa ttt 293 5 275 DNA Homo sapien 5 cgaggtttgg aatcagactt ctgtgtccag taaaaaactc ctgcactgaa gtcattgtga 60 cttgagtagt tacagactga ttccagtgaa cttgatctaa tttcttttga tctaatgaat 120 gtgtctgctt accttgtctc cttttaattg ataagctcca agtagttgct aattttttga 180 caactttaaa tgagtttcat tcacttcttt tacttaatgt tttaagtata gtaccaataa 240 tttcattaac ctgttctcaa gtggtttagc tacca 275 6 301 DNA Homo sapien 6 gaggtctggt ttcctgggta tgcctggact gttgcccagt gtaagatctg tgcaagccat 60 attggatgga agtttacggc caccaaaaaa gacatgtcac ctcaaaaatt ttggggctta 120 acgcgatctg ctctgttgcc cacgatccca gacactgaag atgaaataag tccagacaaa 180 gtaatacttt gcttgtaaac agatgtgata gagataaagt tatctaacaa attggttata 240 ttctaagatc tgctttggaa attattgcct ctgatacata cctaagtaaa cataacatta 300 a 301 7 301 DNA Homo sapien 7 gtccagtttg tacacagtga ttccttatgc acgccgaaag ggtttccgta aaaatgacat 60 tatatacaaa tctgtacacc catccaccag agcgattctc cagctcccag agggagttat 120 caacttaaag caggatacct gaggtttcat gtctttagtt gccttatcat aatcccaaat 180 atacatttca gggtttgttt ttgtttttaa agacactttc ctggaatatg tgcactatgg 240 ttaaaattaa aaacaaaagt aataaaataa aatgatcgct ggaaggactg acctccccac 300 c 301 8 301 DNA Homo sapien 8 ctgtcctcat ctctgcaaag ttcagcttcc ttccccaggt ctctgtgcac tctgtcttgg 60 atgctctggg gagctcatgg gtggaggagt ctccaccaga gggaggctca ggggactggt 120 tgggccaggg atgaatattt gagggataaa aattgtgtaa gagccaaaga attggtagta 180 gggggagaac agagaggagc tgggctatgg gaaatgattt gaataatgga gctgggaata 240 tggctggata tctggtacta aaaaagggtc tttaagaacc tacttcctaa tctcttcccc 300 a 301 9 301 DNA Homo sapien 9 gaggtctgcc taagtagagg acaaagactt cctcctttca aaggagaact gagcccagga 60 ttggtaagtt taaggcactt aaccttgacc agctctgtag gtctggagca ttctggtccc 120 tggccgcttt caccaccagg cccttctcac ttatccacct cacatactgc cccagcattc 180 ctttggcatt gcgagctgtg acttgacaca ttttaatgac aagattgaag tagctacctt 240 gcaggataga ttttctgggg tataggggac aaaccaacag tgccatcagg tgtcttaaca 300 c 301 10 301 DNA Homo sapien 10 ggcaggtcca acagttcttc cagttctggt cgagctttga atcgtccctt gaagtcttct 60 tcagtgtgct ccttcactga cagtctgact ccttcaggaa gactgctttg gattatttcc 120 aagaaaattt ctgcaaacgt agcactcaaa ccgctgatct gaaccactcg ctcatgggtg 180 gtaagcactg agtccaggag cattttgctg ccttggtcct gcaactgcaa cacttctatg 240 gttttggttg gcattgcata actttcctcg actttaatgg agagagattg cagaggttgt 300 g 301 11 301 DNA Homo sapien 11 aggtctgtga ctttcaccca ggacccagga cgcagccctc cgtgggcact gccggcgcct 60 tgtctgcaca ctggaggtcc tccattacag aggcccagcg cacatcgctg gccccacaaa 120 cgttcagggg tacagccatg gcagctcctt cctctgccgt gagaaaagtg cttggagtac 180 ggtttgccac acacgtgact ggacagtgtc caattcaaat ctttcagggc agagtccgag 240 cagcgcttgg tgacagcctg tcctctcctg ctctccaaag gccctgctcc ctgtcctctc 300 t 301 12 301 DNA Homo sapien 12 gaggtctggg attacaggca cgtgccacca cacctagcta atttttgagc atggggctca 60 aaggaactgc tctctggggc atgtcagatt tcggatttgg ggctgcacac tgatactctc 120 taagtggtgg aggaacttca tcccactgaa attcctttgg catttggggt tttgtttttc 180 tttttttcct tcttcatcct cctccttttt taaaagtcaa cgagagcctt cgctgactcc 240 accgaagaag tgcaccactg ggagccaccc cagtgccagg cgcccgtcca gggacacaca 300 c 301 13 256 DNA Homo sapien 13 ttttttggca taaaaaacac aatgatttaa tttctaaagc acttatatta ttatggcatg 60 gtttgggaaa caggttatta tattccacat aggtaattat gcagtgcttc tcatggaaaa 120 aatgcttagg tattggcctt ttctctggaa accatatttt tcctttttta ataatcaact 180 aaaatgtata tgttaaaaag cctcatcttt tgattttcaa tatacaaaat gctttcttta 240 aaagaacaag attcaa 256 14 301 DNA Homo sapien 14 ggtccttgat agaggaagag gaatatccaa ggcaaagcca ccaccacgtc caacctcctc 60 atcctctacc tttcctgtcc ccagaggtat gagatagacc ccctggcctg gttcctgcac 120 tgtgctaggc ccacagtgga cacttccacc ttaatggaga ataggcccca tggagtggag 180 gtccctcctc catggcctgc aacccaatga ctatgggggt gacacaagtg acctctgccc 240 tgtgatggct caacaccatc acacgcaact gtccagacaa gccccctcaa cgggctgctg 300 t 301 15 259 DNA Homo sapien 15 gtcttgaaag tatttattgt ttaataattc tttctcccct cagccccatc cggccactct 60 ctctttctgc ttttctgatc atcctaaagg ctgaatacat cctcctcctg tgtggaggac 120 acgaagcaat actaaaatca atacactcga tcaggtcttc atcagatacc acgtcactgt 180 gggtagagtg ctaattttca acaaatgtgg tgttcttagg gccccacaag gtagtccttt 240 ctcaaggtcg ctgggccac 259 16 301 DNA Homo sapien 16 cgaggttgtt cacattttca aataaataat actccccgta agtaataact gcaaccaatc 60 agtgttattc agtgctatgc ctccttgtaa tgggtagtta ttaattattt tcagagcttt 120 ctggaaatac tgtcctaact ggctatgttt aggatctttg ttatctctga agacaaagaa 180 agaactagga ctcttaattt tggggtgctt cttgactctt agttgggaaa ctgaaaatat 240 ttccaacctt ttacccacgt caatggcata ttctgggaat caccaccacc accaccacta 300 c 301 17 301 DNA Homo sapien 17 gcccgggcag gtctggggcc tagggtggct ctttgcaaag ctgaggggca agctaaggaa 60 gccaggcagg tcaggggccc tttcggcctt ctcaagcctc cacctgagtt ctcgtcaatg 120 ccagtctccc tggtatgatt ggggacatta tcagagaaac atctaatagc gcacatctgg 180 gcacccacac tctgcttcag ttgcatccat cctcccaccc caaattcaac tcctgaccca 240 atacaaaaga cttttttaac caggatttct tcttgcagga aagctgactt ggaaacacgg 300 g 301 18 301 DNA Homo sapien 18 attacaggca cgtgccacca cacctagcta atttttgagc atggggctca aaggaactgc 60 tctctggggc atgtcagatt tcggatttgg ggctgcacac tgatactctc taagtggtgg 120 aggaacttca tcccactgaa attcctttgg catttggggt tttgtttttc tttttttcct 180 tcttcatcct cctccttttt taaaagtcaa cgagagcctt cgctgactcc accgaagaag 240 tgcaccactg gggaccaccc agtgccaggc gcccgtccag ggacacacac agtcttcact 300 g 301 19 301 DNA Homo sapien 19 agaatctctg cactgtcatc aggtacaaca aaagatcaaa cccctgtccc gatgttaact 60 ttttaactta aaagaatgcc agaaaaccca gatcaacact ttccagctac gagccgtcca 120 caaaggccac ccaaaggcca gtcagactcg tgcagatctt attttttaat agtagtaacc 180 acaatacaca gctctttaaa gctgttcata ttcttccccc attaaacacc tgccccgggc 240 ggccaagggc gaattctgca gatatccatc acactggcgg ccgctcgagc atgcatctag 300 a 301 20 290 DNA Homo sapien 20 aggttttttt tttttttttt tttttttttt tttttccctt tcaattcatt taatttcaac 60 aatctgtcaa aaaacagcca ataaacaaat actgaattac attctgctgg gttttttaaa 120 ggctctaaac tataaaaaca tcttgtgtct cccaccctga ccaccctgct acttttccat 180 ataccacagg ccacccataa acacaaagcc agggggtgaa gctgacatgg tctatttgga 240 gccagtaaac aggagggcga taagtcctga taagcactta tggacaatat 290 21 301 DNA Homo sapien 21 agaaaggtaa ctgccagcca ggcttgcatt gtttagccag aaattgctgc ttggttctag 60 actctttaaa aaaaaaaaat acccagggtt tgtcatcatt ttcagaggca gagtgccaaa 120 tatcacccaa agctcttgtg tctttttttt acccccttat tttattttta tttattaatt 180 ttttgtgcaa acatcaaatg tcactggtgt tcacagaagg cttttttgac tagccttaaa 240 ttcctgagtc aaaagattaa tcagattttc aggcagtgtt taatcaggtg ctttgtcctg 300 t 301 22 301 DNA Homo sapien 22 gacgccatgc accctccggt aaccagcagc cgcctgtcca tcccccaaga ccggaaaggc 60 agcagcagcc cccgggagcc cagggctgtc ctcggtgcat ctggctgcag agggaaattg 120 atgaccttac acagcaacta gcggccatgc agtccttcac tgacaagttc caggaccttt 180 gaagttggag ccagcgtccg gagctgcagc caagcgagtt tcctccttat cctccttagc 240 cagggctttt tctcttccgc tgcatttgcc cccttcccaa cgcaattcaa agcagttgtg 300 a 301 23 381 DNA Homo sapien 23 cgaggtccag acagtggacc aagagatacg ctacataaat tggggtttca caattcttac 60 attatttgtc tgtcacagaa gagagctgct tatgattttg aaggggtcag ggagggtggg 120 agttggtaaa gagtagggta tttctataac agatattatt cagtcttatt tcctaagatt 180 ttgttgtaac ttaaggtatc ttgctacagt agacagaatt ggtaatagca acttttaaaa 240 ttgtcattag ttctgcaata ttagctgaaa tgtagtacag aaaagaatgt acatttagac 300 atttgggttc agttgcttgt agtctgtaaa tttaaaacag cttaatttgg tacaggttac 360 acatatggac ctcccgggcg g 381 24 214 DNA Homo sapien 24 aatgatgtaa aaattaatca acagggctgc cacttgcgaa tcccctccaa ggatgctgtg 60 caaagggtct cattggtcct gatgaataat cttgtgactg tacatattcc tgggtgcatg 120 tccacaaata ctgaggtata gcctgcatgc cactaaaaat aacaaaggtt tcaggggtgg 180 aaacattgtc caccacactg tcatgaccat cttt 214 25 302 DNA Homo sapien 25 gggggcactg agaactccct ctggaattct tggggggtgt tggggagaga ctgtgggcct 60 ggagataaaa cttgtctcct ctaccaccac cctgtaccct agcctgcacc tgtcctcatc 120 tctgcaaagt tcagcttcct tccccaggtc tctgtgcact ctgtcttgga tgctctgggg 180 agctcatggg tggaggagtc tccaccagag ggaggctcag gggactggtt gggccaggga 240 tgaatatttg agggataaaa attgtgtaag aagccaaaga aattggtagt aggggggaga 300 ac 302 26 301 DNA Homo sapien 26 ttggagaacg cgctgacata ctgctcggcc acagtcagtg aagctgctgc atctccatta 60 tgttgtgtca gagctgcagc caggattcga atagcttcag ctttagcctt ggccttcgcc 120 agaactgcac tggcctctcc tgctgcctga tttatctgtg cagccttttc tgcttcggag 180 gccaggatct gggcctgttt cttcccttct gccacattga tggccgactc tcgggtcccc 240 tcagactcta gaactgtggc ccgtttccgc cgctctgcct ccacctgcat ctgcatagac 300 t 301 27 301 DNA Homo sapien 27 aaatcagtca tcacatctgt gaaaagagtg ctagttataa caaatgagat cacaaatttg 60 accattttat tagacaccct ctattagtgt taacagacaa agatgaaggt taagttgaaa 120 tcaaattgaa atcatcttcc ctctgtacag attgcaatat ctgataatac cctcaacttt 180 cttggtgcaa attaattgcc tggtactcac agtccagtgt taacaggcaa taatggtgtg 240 attccagagg agaggactag gtggcaggaa aataaatgag attagcagta tttgacttgg 300 a 301 28 286 DNA Homo sapien 28 tttttttttg cacaggatgc acttattcta ttcattctcc cccacccttc ccatatttac 60 atccttagag gaagagaggg gtaaggtgat aaagtaactg aaggaccgca agacgggtat 120 gtcccttgtt caccaaatgg tcaaagggtc aaagatcgga ggaggtcagg gggtaacgca 180 ggaacaggtg agggcgtttc gccctctctc cctctcccct tttcaacctc ttaatcactg 240 gctaactcgc gacctcatgg gttaattcgt aagcttacac gcgttg 286 29 301 DNA Homo sapien 29 gtcatgttct tgctcttcct tctttacaca tttgagttgt gccttctgtt cttaaagaga 60 ttttcctttg ttcaaaggat ttattcctac catttcacaa atccgaaaat aattgaggaa 120 acaggttaca tcattccaat tttgccttgg gtttgaagag tctctcatgg tggcacagtc 180 ctccagggta gctatgttgt tgggctcccc tacatcccag aagctcagag actttgtcaa 240 aggtgtgccg tccacccatt gccactgacc ctcgacaacc tggtctgaca gtccaataaa 300 a 301 30 332 DNA Homo sapien 30 gagcagaatt gatgcctatg gctccaagtc aaatactgct aatctcattt attttcctgc 60 cacctagtcc tctcctctgg aatcacacca ttattgcctg ttaacactgg actgtgagta 120 ccaggcaatt aatttgcacc aagaaagttg agggtattat cagatattgc aatctgtaca 180 gagggaagat gatttcaatt tgatttcaac ttaaccttca tctttgtctg ttaacactaa 240 tagagggtgt ctaataaaat ggtcaaattt gtgatctcat ttgttataac tagcactctt 300 ttcacagatg tgatgactga tttccagcag ac 332 31 141 DNA Homo sapien 31 aaaggctatc aagtactttg aaggacagga aggaatgaac acacccaggt ggacgtttgg 60 tttcatttgc aggggttcag ggagggttgc aggggttcag ggagggctct tgtcccacaa 120 ccgggggaag ggagagggca c 141 32 201 DNA Homo sapien 32 gagctgatct cacagcacat acagaatgat gctactatgt agaccctcac tcccttggga 60 aatctgtcat ctaccttaaa gagagaaaaa agatggaaca taggcccacc tagtttcatc 120 catccaccta cataaccaac atagatgtga ggtccactgc actgatagcc agactgcctg 180 gggtaaacct tttcagggag g 201 33 181 DNA Homo sapien 33 tttcaaaaca ctcatatgtt gcaaaaaaca catagaaaaa taaagtttgg tgggggtgct 60 gactaaactt caagtcacag acttttatgt gacagattgg agcagggttt gttatgcatg 120 tagagaaccc aaactaattt attaaacagg atagaaacag gctgtctggg tgaaatggtt 180 c 181 34 151 DNA Homo sapien 34 atgtcctgca cagtatagct tggacctctg ggcctgaacc agggtgagca tcaaggcccc 60 catttctcct caccacgggg tcgcttgtca gctccaagaa ccagtctggc cccactgaga 120 acttttcagt cgagggcctg atgaatcttg g 151 35 291 DNA Homo sapien 35 tctttagggc aaaatcatgt ttctgtgtac ctagcaatgt gttcccattt tattaagaaa 60 agctttaaca cgtgtaatct gcagtcctta acagtggcgt aattgtacgt acctgttgtg 120 tttcagtttg tttttcacct ataatgaatt gtaaaaacaa acatacttgt ggggtctgat 180 agcaaacata gaaatgatgt atattgtttt ttgttatcta tttattttca tcaatacagt 240 attttgatgt attgcaaaaa tagataataa tttatataac aggttttctg t 291 36 201 DNA Homo sapien 36 ctgatacaat tataataacg gttccctgaa ccttttagag tgcaattaag aacaaaaact 60 aaattttgtt tacatgaata tggaataaat acaataatca aaatatgact ctccctaaaa 120 gtgaaacaca caagccaatc cggaactgct gtgcgaaaga taaaatcgag aaaggcaagg 180 tttcggtagg aggacgcgat g 201 37 121 DNA Homo sapien 37 catcacactg gcggccgctc gagcatgcat ctagagggcc caattcgccc tataatgagt 60 cgtattacaa ttcactggcc gtcgttttac aacgtcgtga ctgggaaaac cctggcgtta 120 c 121 38 200 DNA Homo sapien 38 aaacatgtat tactctatat ccccaagtcc tagagcatga cctgcatgtt ggagatgttg 60 tacagcaatg tatttatcca gacatacata tatgatattt agagacacag tgattctttt 120 gataacacca cacatagaac attataatta cacacaaatt tatggtaaaa gaattaatat 180 gctgtctggt gctgctgtta 200 39 760 DNA Homo sapien 39 gcgtggtcgt cggccgaggt cctgggctag acctaatggt ttattattgg tggagagaaa 60 gatctggaaa tacttgaggt tattacatac tagattagct tctaatgtga accatttttc 120 ttttaacagt gatcaaatta ttatttcgaa gttaatcgtt cccttggtgg ctgcatacac 180 atcgcattaa caaacatact gttgtatttt ttcccagttt tgtttggcta tgccaccaca 240 gtcatcccca gggtctatac atactatgtt tcaactgtat tatttgccat ttttggcatt 300 agaatgcttc gggaaggctt aaagatgagc cctgatgagg gtcaagagga actggaagaa 360 gttcaagctg aattaaagaa gaaagatgaa gaagtaagcc atggcactgt tgatctggac 420 caaaaaggca ctcaactagg aataaacact ctacagaggt ttctcagtgg ccccatctgt 480 gtgatatgcg gggctacaca aaaatagctt cttttgcttt gttctgttct tatacctgtc 540 tgtgatctga cttggggttg gtgtgaatgt agtagagaaa ggaagctgac agatgaatac 600 tgaacacagg taatcagttt ccttaattag gttgattata agctcctgaa aagcaggaac 660 tgtattttat aattttacct gtttctcccg tggtgtctag gatagtaagt gagcagagca 720 gtaaatactg tttggtttgt tcagacctgc ccgggcggcc 760 40 452 DNA Homo sapien 40 aatcactaaa gatattgact agagaatgct gtgtgctatt tcaattacat ttgtttttct 60 tttattaaca ggaattttga ttcttcaagg aagtggctca atttcaattt caggtgacca 120 ggtttatcgt gacttttcct tcttgtttac ttttcgctag gaaggggagt tgtaggggca 180 gattcaggta ttggaatagg aaaattacgt ctaaaccatg gaaatcttgg aaatggaatt 240 ggtggaagtg ggcgaaatgg atatgggtaa gggaacacaa aaaaccctga agctaattca 300 tcgctgtcac tgatacttct tttttctcgt tcctggtctt gagagactgg gaaaccaaca 360 gccactgcca agatggctgt gatcaggagg agaactttct tcatctcaaa cgtttcagtc 420 agttctttct ctcacctcgg ccgcgaccac gc 452 41 676 DNA Homo sapien 41 aatctttgaa tgccaagtct cttctgtact ttcttttatt aacatcatag tctttgcatc 60 aagatacata gcaatgatag caggtttctt tttaaagctt agtattaata ttaaatattt 120 ttccccattt aaattttaca ttacttgcca agaaaaaaaa aaaattaaaa ctcaagttac 180 ttgaagcctg gacacacttc catgattagc cgggctaggt aaaagttggt ggctttattc 240 ttcctgctct ataagcagat ccaggcccta gaaagatggg accagggtat ataattgttt 300 ttgaaaagtg tgctacaaaa atggatggcc tgttataagc caggatacaa agttaaggat 360 gggggtaagg gagggacatt ttcttccaga agaaaagaca gaatttctga agagtcccag 420 tccataattt tcccaaaatg gttggaggag agggtaaaat ctcaacatga gtttcaaagt 480 actgtctctg tgaggggccg gtagatgcct tgctgaggag ggatggctaa tttggaccat 540 gccccatccc cagctaggag aatggaaatg gaaactttaa ttgcccagtg ggtgtgaaag 600 tgggctgaag cttggttggt actgaattct ctaagaggtt tcttctagaa acagacaact 660 cagacctgcc cgggcg 676 42 468 DNA Homo sapien 42 agcgtggtcg cggccgaggt ttggccggga gcctgatcac ctgccctgct gagtcccagg 60 ctgagcctca gtctccctcc cttggggcct atgcagaggt ccacaacaca cagatttgag 120 ctcagccctg gtgggcagag aggtagggat ggggctgtgg ggatagtgag gcatcgcaat 180 gtaagactcg ggattagtac acacttgttg attaatggaa atgtttacag atccccaagc 240 ctggcaaggg aatttcttca actccctgcc ccccagccct ccttatcaaa ggacaccatt 300 ttggcaagct ctatgaccaa ggagccaaac atcctacaag acacagtgac catactaatt 360 aaaaccccct gcaaagccca gcttgaaacc ttcacttagg aacgtaatcg tgtcccctat 420 cctacttccc cttcctaatt ccacagacct gcccgggcgg ccgctcga 468 43 408 DNA Homo sapien 43 atcatatcaa aacactatct tcccatctgt ttctcaatgc ctgctacttc ttgtagatat 60 ttcatttcag gagagcagca gttaaacccg tggattttgt agttaggaac ctgggttcaa 120 acctctttcc actaattggc tatgtctctg gacagttttt tttttttttt ttttttttaa 180 accctttctg aactttcact ttctatggct acctcaaaga attgttgtga ggcttgagat 240 aatgcatttg taaagggtct gccagatagg aagatgctag ttatggattt acaaggttgt 300 taaggctgta agagtctaaa acctacagtg aatcacaatg catttacccc cactgacttg 360 gacataagtg aaaactagcc cgaagtctct ttttcaaatt acttacag 408 44 160 DNA Homo sapien 44 tggtcgcggc cgaggtcttg tgtgccctgt ggtccagggg accaagaaca acaagatcca 60 ctctctgtgc tacaatgatt gcaccttctc acgcaacact ccaaccagga ctttcaacta 120 caacttctcc gctttggcaa acaccgtcac tcttgctgga 160 45 231 DNA Homo sapien 45 cgagcggccg cccgggcagg tctggggagg tgattccatc cagagtcata tctgttgtca 60 ccccaataag tcgatcagca aggctgacag gctgtgagga aaccccggcc ttgtagcctg 120 tcacctctgg ggggatgatg actgcctggc agacgtaggc tgtgatagat ttgggagaaa 180 acctgactca ccctcaggaa tccggaggtc ggtgacattg tcggtgcaca c 231 46 371 DNA Homo sapien 46 cccgggcagg tctgtgtaac atgccaaggc tttgcacttt ctgcagagca gttttttatt 60 ttccttatca ggtacaggtt ttggtttttc ttgactatct ctgatgaatt tttcatgagt 120 ctgtatatgc agaatctttt ccctaaatac tgcttcgtcc catgtctgaa ggcgtaaaat 180 aaagtcattc atcatttttt ctttgtacat gtttatttgt tctttttcaa ttacaccaag 240 cattactagt cagaaggaag cacttgctac ctcttgctct tcctctgcct ctggtttgga 300 tcattttgat gacattgccc acattactca tgaaggatga caagattgca ctgtgcaatg 360 tcaattgcct t 371 47 261 DNA Homo sapien 47 gccctgtttt tatacacttc acatttgcag aaatataatg atgccctcat tatcagtgag 60 catgcacgaa tgaaagatgc tctggattac ttgaaagact tcttcagcaa tgtccgagca 120 gcaggattcg atgagattga gcaagatctt actcagagat ttgaagaaaa gctgcaggaa 180 ctagaaagtg tttccaggga tcccagcaat gagaatccta aacttgaaga cctctgcttc 240 atcttacaag aagagtacca c 261 48 701 DNA Homo sapien 48 cgagcggccc ccgggcaggt ccaattagta caagtctcat gatataatca ctgcctgcat 60 acatatgcac agatccagtt agtgagtttg tcaagcttaa tctaattggt taagtctcaa 120 agagattatt attcttgatg tttgctttgt attggctaac aaatgtgcag aggtaataca 180 tatgtgatgt ccgatgtctc tgtctttttt tttgtcttta aaaaataatt ggcagcaact 240 gtatttgaat aaaatgattt cttagtatga ttgtaccgta atgaatgaaa gtggaacatg 300 tttctttttg aaagggagag aattgaccat ttattattgt gatgtttaag ttataactta 360 ttgagcactt ttagtagtga taactgtttt taaacttgcc taataccttt cttgggtatt 420 gtttgtaatg tgacttattt aacccccttt tttgtttgtt taagttgctg ctttaggtta 480 acagcgtgtt ttagaagatt taaatttttt tcctgtctgc acaattagtt attcagagca 540 agagggcctg attttataga agccccttga aaagaggtcc agatgagagc agagatacag 600 tgagaaatta tgtgatctgt gtgttgtggg aagagaattt tcaatatgta actacggagc 660 tgtagtgcca ttagaaactg tgaatttcca aataaatttg a 701 49 270 DNA Homo sapien 49 agcggccgcc cgggcaggtc tgatattagt agctttgcaa ccctgataga gtaaataaat 60 tttatgggcg ggtgccaaat actgctgtga atctatttgt atagtatcca tgaatgaatt 120 tatggaaata gatatttgtg cagctcaatt tatgcagaga ttaaatgaca tcataatact 180 ggatgaaaac ttgcatagaa ttctgattaa atagtgggtc tgtttcacat gtgcagtttg 240 aagtatttaa attaaccact cctttcacag 270 50 271 DNA Homo sapien 50 atgcatttat ccatatgaac ttgattattc tgaattactg actataaaaa ggctattgtg 60 aaagatatca cactttgaaa cagcaaatga attttcaatt ttacatttaa ttataagacc 120 acaataaaaa gttgaacatg cgcatatcta tgcatttcac agaagattag taaaactgat 180 ggcaacttca gaattatttc atgaagggta caaacagtct ttaccacaat tttcccatgg 240 tcttatcctt caaaataaaa ttccacacac t 271 51 241 DNA Homo sapien 51 tggtcgcggc cgaggtgtga ggagatgaac tttgtgttaa tggggggcac tttaaatcga 60 aatggcttat ccccaccgcc atgtaagtta ccatgcctgt ctcctccctc ctacacattt 120 ccagctcctg ctgcagttat tcctacagaa gctgccattt accagccctc tgtgattttg 180 aatccacgag cactgcaggc cctccacagc gttactaccc agcaggcact cagctcttca 240 t 241 52 271 DNA Homo sapien 52 tccaagactt aaaacttagg aaacacctat gatgccactt taactggaag taatggagac 60 atctgattcc aaattcacat tttaaatgcc tatttgcaat cagcaaagag ccaggtatgc 120 tgcatgctgc ttgctgtaag ttacgatttg gcttcactag ctcaaatttt ttcactccac 180 caaaagataa ggcacaggcc cgtttgtcca atcaagtttg ctgaaaatac tgcagcctga 240 gtgtagacaa acttcccctg aatttgctag a 271 53 493 DNA Homo sapien 53 ttagcgtggt cgcggtccga ggtctggcct gactagctca ctctgaagag tgtctttcac 60 atggattaac caaaaaatgc attactgcct ttggcacact gtcttgaata ttctttctga 120 caatgagaaa atatgattta atggagtcgt tcaataacct cacaatctcg ctgttccgag 180 cagatagttt tcgtgccaac aggaactggc acatctagca ggttcacggc atgacctttt 240 tgtggactgg ctggcataat tggaatgggt tttgattttt cttctgctaa taactcttca 300 agcttttgaa gttttcaagc attcctctcc agttgcctgt ggttggttct tgaacaccat 360 ctccaacccc accacctcca gatgcaacct tgtctcgtga tacagacctg cccgggcggc 420 cctcaagggc gaattctgca gatatccatc acactggcgg ccgctcgagc atgcatctag 480 agggcccaat tcg 493 54 321 DNA Homo sapien 54 cgtggtcgcg gccgaggtct gtttgcttgt tggtgtgagt ttttcttctg gagactttgt 60 actgaatgtc aataaactct gtgattttgt taggaagtaa aactgggatc tatttagcca 120 ctggtaagct tctgaggtga aggattcagg gacatctcgt ggaacaaaca ctccccactg 180 gactttctct ctggagatac ccttttgaat atacaatggc cttggctcac taggtttaaa 240 tacaaacaag tctgaaaccc actgaagact gagagattgc agcaatattc tctgaattag 300 gatcgggttc cataactcta a 321 55 281 DNA Homo sapien 55 ttgcaaatga aactgtggat gtataataag aaaacacaag ggtttattct taacactaaa 60 attaacatgc cacacgaaga ctgcattaca gctctctgtt tctgtaatgc agaaaaatct 120 gaacagccca ccttggttac agctagcaaa gatggttact tcaaagtatg gatattaaca 180 gatgactctg acatatacaa aaaagctgtt ggctggacct gtgactttgt tggtagttat 240 cacaagtatc aagcaactaa ctgttgtttc tccgaagatg g 281 56 612 DNA Homo sapien 56 gcgtggtcgc ggccgaggtc ctgtccgggg gcactgagaa ctccctctgg aattcttggg 60 gggtgttggg gagagactgt gggcctggag ataaaacttg tctcctctac caccaccctg 120 taccctagcc tgcacctgtc ctcatctctg caaagttcag cttccttccc caggtctctg 180 tgccactctg tcttggatgc tctggggagc tcatgggtgg aggagtctcc accagaggga 240 ggctcagggg actggttggg ccagggatga atatttgagg gataaaaatt gtgtaagagc 300 caaagaattg gtagtagggg gagaacagag aggagctggg ctatgggaaa tgatttgaat 360 aatggagctg ggaatatggc tggatatctg gtactaaaaa agggtcttta agaacctact 420 tcctaatctc ttccccaatc caaaccatag ctgtctgtcc agtgctctct tcctgcctcc 480 agctctgccc caggctcctc ctagactctg tccctgggct agggcagggg aggagggaga 540 gcagggttgg gggagaggct gaggagagtg tgacatgtgg ggagaggacc agacctgccc 600 gggcggccgt cg 612 57 363 DNA Homo sapien 57 gtcgcggccg aggtcctgag cgtcacccta gttctgcccc tttttagctg tgtagacttg 60 gacaagacat ttgacttccc tttctccttg tctataaaat gtggacagtg gacgtctgtc 120 acccaagaga gttgtgggag acaagatcac agctatgagc acctcgcacg gtgtccagga 180 tgcacagcac aatccatgat gcgttttctc cccttacgca ctttgaaacc catgctagaa 240 aagtgaatac atctgactgt gctccactcc aacctccagc gtggatgtcc ctgtctgggc 300 cctttttctg ttttttattc tatgttcagc accactggca ccaaatacat tttaattcac 360 cga 363 58 750 DNA Homo sapien 58 cgtggtcgcg gccgaggtct aattccacct gactggcaga acctgcgccc ctcgcctaac 60 ctgcgccctt ctcccaactc gcgtgcctca cagaacccag gtgctgcaca gccccgagat 120 gtggcccttc ttcaggaaag agcaaataag ttggtccaag tacttgatgc ttaaggaata 180 cacaaaggtg cccatcaagc gctcagaaat gctgagagat atcatccgtg aatacactga 240 tgtttatcca gaaatcattg aacgtgcatg ctttgtccta gagaagaaat ttgggattca 300 actgaaagaa attgacaaag aagaacacct gtatattctc atcagtaccc ccgagtccct 360 ggctggcata ctgggaacga ccaaagacac acccaagctc ggtctcttct tggtgattct 420 gggtgtcatc ttcatgaatg gcaaccgtgc cagtgaggct gtcttttggg aggcactacg 480 caagatggga ctgcgtcctg gggtgagaca tcccctccct tggagatcta aggaaacttc 540 tcacctatga gtttgtaaag cagaaatacc tggactacag acgagtgccc aacagcaacc 600 ccccggagta tgagttcctc tggggcctcc gtccctacca tgagactagc aagatgaaaa 660 tgctgagatt cattgcagag gttcagaaaa gagaccctcg tgactggact gcacagttca 720 tggaggctgc agatgaggac ctgcccgggc 750 59 505 DNA Homo sapien 59 tggccgcccg ggcaggtcca gtctacaagc agagcactct catggggagc accagatgag 60 ttccagccgc agttctttta taagctttaa gtgcctcatg aagacgcgag gatctcttcc 120 aagtgcaacc tggtcacatc agggcacatt cagcagcaga agtctgtttc cagtatagtc 180 cttggtatgg ctaaattcca ctgtcccttt ctcagcagtc aataatccat gataaattct 240 gtacaacact gtagtcaata acagcagcac cagacagcat attaattctt ttaccataaa 300 tttgtgtgta attataatgt tctatgtgtg gtgttatcaa aagaatcact gtgtctctaa 360 atatcatata tgtatgtctg gataaataca ttgctgtaca acatctccaa catgcaggtc 420 atgctctaag acttggggat atagagtaat acatgtttcg tggacctcgg ccgcgaccac 480 gctaagggcg aattctgcag atatc 505 60 520 DNA Homo sapien 60 cgtggtcgcg gccgaggtcc tcaggacaag gaaacaggta tcagcatgat ggtagcagaa 60 accttatcac caaggtgcag gagctgactt cttccaaaga gttgtggttc cgggcagcgg 120 tcattgcctg cccttgctgg agggctgatt ttagtgttgc ttattatgtt ggccctgagg 180 atgcttcgaa gtgaaaataa gaggctgcag gatcagcggc aacagatgct ctcccgtttg 240 cactacagct ttcacggaca ccattccaaa aaggggcagg ttgcaaagtt agacttggaa 300 tgcatggtgc cggtcagtgg gcacgagaac tgctgtctga cctgtgataa aatgagacaa 360 gcagacctca gcaacgataa gatcctctcg cttgttcact ggggcatgta cagtgggcac 420 gggaagctgg aattcgtatg acggagtctt atctgaacta cacttactga acagcttgaa 480 ggacctgccc gggcggccgc tcgaaagggg cgaattctgc 520 61 447 DNA Homo sapien 61 agagaggtgt ttttattctt tggggacaaa gccgggttct gtgggtgtag gattctccag 60 gttctccagg ctgtagggcc cagaggctta atcagaattt tcagacaaaa ctggaacctt 120 tcttttttcc cgttggttta tttgtagtcc ttgggcaaac caatgtcttt gttcgaaaga 180 gggaaaataa tccaaacgtt tttcttttaa cttttttttt aggttcaggg gcacatgtgt 240 aggcttgcta tataggtaaa ttgcatgtca ccagggtttg ttgtacagat tatttcatca 300 tccagataaa aagcatagta ccagataggt agttttttga tcctcaccct ccttccatgc 360 tccgacctca ggtaggcccc agtgtctgac ctgcccggcg gcccgctcga aagggccaat 420 tctgcagata tccatcacac tggccgg 447 62 83 PRT Homo sapien 62 Lys Lys Val Leu Leu Leu Ile Thr Ala Ile Leu Ala Val Ala Val Gly 1 5 10 15 Phe Pro Val Ser Gln Asp Gln Glu Arg Glu Lys Arg Ser Ile Ser Asp 20 25 30 Ser Asp Glu Leu Ala Ser Gly Phe Phe Val Phe Pro Tyr Pro Tyr Pro 35 40 45 Phe Arg Pro Leu Pro Pro Ile Pro Phe Pro Arg Phe Pro Trp Phe Arg 50 55 60 Arg Asn Phe Pro Ile Pro Ile Pro Ser Ala Pro Thr Thr Pro Leu Pro 65 70 75 80 Ser Glu Lys 63 683 DNA Homo sapien 63 acaaagattg gtagctttta tattttttta aaaatgctat actaagagaa aaaacaaaag 60 accacaacaa tattccaaat tataggttga gagaatgtga ctatgaagaa agtattctaa 120 ccaactaaaa aaaatattga aaccactttt gattgaagca aaatgaataa tgctagattt 180 aaaaacagtg tgaaatcaca ctttggtctg taaacatatt tagctttgct tttcattcag 240 atgtatacat aaacttattt aaaatgtcat ttaagtgaac cattccaagg cataataaaa 300 aaagwggtag caaatgaaaa ttaaagcatt tattttggta gttcttcaat aatgatrcga 360 gaaactgaat tccatccagt agaagcatct ccttttgggt aatctgaaca agtrccaacc 420 cagatagcaa catccactaa tccagcacca attccttcac aaagtccttc cacagaagaa 480 gtgcgatgaa tattaattgt tgaattcatt tcagggcttc cttggtccaa ataaattata 540 gcttcaatgg gaagaggtcc tgaacattca gctccattga atgtgaaata ccaacgctga 600 cagcatgcat ttctgcattt tagccgaagt gagccactga acaaaactct tagagcacta 660 tttgaacgca tctttgtaaa tgt 683 64 749 DNA Homo sapien misc_feature (1)...(749) n = A,T,C or G 64 ctgttcattt gtccgccagc tcctggactg gatgtgtgaa aggcatcaca tttccatttt 60 cctccgtgta aatgttttat gtgttcgcct actgatccca ttcgttgctt ctattgtaaa 120 tatttgtcat ttgtatttat tatctctgtg ttttccccct aaggcataaa atggtttact 180 gtgttcattt gaacccattt actgatctct gttgtatatt tttcatgcca ctgctttgtt 240 ttctcctcag aagtcgggta gatagcattt ctatcccatc cctcacgtta ttggaagcat 300 gcaacagtat ttattgctca gggtcttctg cttaaaactg aggaaggtcc acattcctgc 360 aagcattgat tgagacattt gcacaatcta aaatgtaagc aaagtaagtc attaaaaata 420 caccctctac ttgggcttta tactgcatac aaatttactc atgagccttc ctttgaggaa 480 ggatgtggat ctccaaataa agatttagtg tttattttga gctctgcatc ttancaagat 540 gatctgaaca cctctccttt gtatcaataa atagccctgt tattctgaag tgagaggacc 600 aagtatagta aaatgctgac atctaaaact aaataaatag aaaacaccag gccagaacta 660 tagtcatact cacacaaagg gagaaattta aactcgaacc aagcaaaagg cttcacggaa 720 atagcatgga aaaacaatgc ttccagtgg 749 65 612 DNA Homo sapien 65 acagcagcag tagatggctg caacaacctt cctcctaccc cagcccagaa aatatttctg 60 ccccacccca ggatccggga ccaaaataaa gagcaagcag gcccccttca ctgaggtgct 120 gggtagggct cagtgccaca ttactgtgct ttgagaaaga ggaaggggat ttgtttggca 180 ctttaaaaat agaggagtaa gcaggactgg agaggccaga gaagatacca aaattggcag 240 ggagagacca tttggcgcca gtcccctagg agatgggagg agggagatag gtatgagggt 300 aggcgctaag aagagtagga ggggtccact ccaagtggca gggtgctgaa atgggctagg 360 accaacagga cactgactct aggtttatga cctgtccata cccgttccac agcagctggg 420 tgggagaaat caccattttg tgacttctaa taaaataatg ggtctaggca acagttttca 480 atggatgcta aaacgattag gtgaaaagtt gatggagaat tttaattcag gggaattagg 540 ctgataccat ctgaaaccat ttggcatcat taaaaatgtg acaacctggt ggctgccagg 600 gaggaagggg ag 612 66 703 DNA Homo sapien 66 tagcgtggtc gcggccgagg tacattgatg ggctggagag cagggttggc agcctgttct 60 gcacagaacc aagaattaca gaaaaaagtc caggagctgg agaggcacaa catctccttg 120 gtagctcagc tccgccagct gcagacgcta attgctcaaa cttccaacaa agctgcccag 180 accagcactt gtgttttgat tcttcttttt tccctggctc tcatcatcct gcccagcttc 240 agtccattcc agagtcgacc agaagctggg tctgaggatt accagcctca cggagtgact 300 tccagaaata tcctgaccca caaggacgta acagaaaatc tggagaccca agtggtagag 360 tccagactga gggagccacc tggagccaag gatgcaaatg gctcaacaag gacactgctt 420 gagaagatgg gagggaagcc aagacccagt gggcgcatcc ggtccgtgct gcatgcagat 480 gagatgtgag ctggaacaga ccttcctggc ccacttcctg atcacaagga atcctgggct 540 tccttatggc tttgcttccc actgggattc ctacttaggt gtctgccctc aggggtccaa 600 atcacttcag gacaccccaa gagatgtcct ttagtctctg cctgaggcct agtctgcatt 660 tgtttgcata tatgagaggg tacctgcccg ggcggccgct cga 703 67 1022 DNA Homo sapien 67 cttgagaaag caggattgtt ttaagttcca agatttaaca aacttactgt tcagcatcat 60 attcaagcct aaaaggaaga taggattttc aagatatatt tccaacttct ttaacatggc 120 accatggatg aactgtttct cagcactgtg ctgcttcact tggaattaag gatgaattgg 180 gaggagacag tatgacatag gtgggtaggt tgggtggtga ggggaaccag ttctaatagt 240 cctcaactcc actccagctg ttcctgttcc acacggtcca ctgagctggc ccagtccctt 300 tcactcagtg tgtcaccaaa ggcagcttca aggctcaatg gcaagagacc acctataacc 360 tcttcacctt ctgctgcctc tttctgctgc cactgactgc catggccatc tgctatagcc 420 gcattgtcct cagtgtgtcc aggccccaga caaggaaggg gagccatggt gagactccaa 480 ttcccaggcc ttaatcctta accctagacc tgttgcctct agcatcattt atttatctac 540 ctacctaata gctatctacc agtcattaaa ccatggtgag attctaacca tgtctagcac 600 ctgatgctag agataatttt gttgaatccc ttcaattata aacagctgag ttagctggac 660 aaggactagg gaggcaatca gtattattta ttcttgaaca ccatcaagtc tagacttggt 720 ggcttcatat ttctatcata atccctgggg gtaagaaatc atatagcccc aggttgggaa 780 ggggaaaacg gtttgcaaca ttctcctcct tgtaggaggc gagctctgtc tcactagcta 840 tgcccctcca tcaattcacc ctatactcag atcagaagct gagtgtctga attacagtat 900 attttctaaa ttcctagccc ctgctggtga atttgccctc ccccgctcct ttgacaattg 960 tccccgtgtt cgtctccggg ccctgagact ggccctgctt atcttgctga ccttcatcct 1020 ct 1022 68 449 DNA Homo sapien 68 ccagatccat tttcagtggt ctggatttct ttttattttc ttttcaactt gaaagaaact 60 ggacattagg ccactatgtg ttgttactgc cactagtgtt caagtgcctc ttgttttccc 120 agagatttcc tgggtctgcc agaggcccag acaggctcac tcaagctctt taactgaaaa 180 gcaacaagcc actccaggac aaggttcaaa atggttacaa cagcctctac ctgtcgcccc 240 agggagaaag gggtagtgat acaagtctca tagccagaga tggttttcca ctccttctag 300 atattcccaa aaagaggctg agacaggagg ttattttcaa ttttattttg gaattaaata 360 cttttttccc tttattactg ttgtagtccc tcacttggat atacctctgt tttcacgata 420 gaaataaggg aggtctagag cttctattc 449 69 387 DNA Homo sapien misc_feature (1)...(387) n = A,T,C or G 69 gcccttagcg tgggtcgcgg cncgangtct ggagcntatg tgatncctat ggtncncagg 60 cnnatactgc tantctcatt tattctcctg cnacctantc ctctnctctg gaatcacacc 120 attattgcct gttaacactg gactgtgagt accangcaat taatttgcac caanaaagtt 180 gagggtatta tcanatattg caatctgtac agagggaaga tgatttcaat ttgatttcaa 240 cttaaccttc atctttgtct gttaacacta atagagggtg tctaataaaa tggcaaattt 300 gngatctcat tnggtataac tacactcttt ttcacagatg tgatgactga atttccanca 360 acctgcccgg gcggncgntc naagggc 387 70 836 DNA Homo sapien 70 tattccattt acaaaataaa ttcagccctg cactttcttt agatgccttg atttccagaa 60 tggagcttag tgctactgaa taccctggcc acagagccac ctcaggatat tcttttctcc 120 accctagttt atttatttat agatatctgt ttacaaagtc tgtagtaaat cctgatgctg 180 accatctgaa atgtactttt tttctgaatg ctgtttcaat ctaaaatagc agcttttgag 240 aaaacaatga tgtaaattcc ttatgataaa aggatgattc tatatattct ttaatgatat 300 taaatatgcc gaagccaagc acacagtctt tctaaagtgt gtgtatgttt gtgtgaatgt 360 gaatgatact gatcttatat ctgttaaaag ttgttttaaa aagctgtggc atcccattgt 420 tcatatttgc caagtcttct gtaaagatgt ctaggacgaa atattttatg tgctaatgca 480 tgtatttgta aaccagattt gtttaccact caaaattaac ttgttttctt catccaaaaa 540 agtttatttc ttccacgtac ttaaattttc tgtgtgggta taatatagct ttctaatttt 600 tttctttcac aaaggcaggt tcaaaattct gttgaaagaa aaatgctttc tgaaactgag 660 gtataacacc agagcttgct gtttaaagga ttatatgatg tacatcagtt ctataaatgt 720 gctcagcagt ttaacatgtg aatcctgttt taaagtgctc agatttcaac tgtgtaagcc 780 attgatataa cgctgtaatt aaaaatgttt atatgaaaaa aaaaaaaaaa aaaaaa 836 71 618 DNA Homo sapien 71 gttgcagtga gctcaagtgt tgggtgtatc agctcaaaac accatgtgat gccaatcatc 60 tccacaggag caatttgttt accttttttt tctgatgctt tactaacttc atcttttaga 120 tttaaatcat tagtagatcc tagaggagcc agtttcagaa aatatagatt ctagttcagc 180 accacccgta gttgtgcatt gaaataatta tcattatgat tatgtatcag agcttctggt 240 tttctcattc tttattcatt tattcaacaa ccacgtgaca aacactggaa ttacaggatg 300 aagatgagat aatccgctcc ttggcagtgt tatactatta tataacctga aaaaacaaac 360 aggtaatttt cacacaaagt aatagatatc atgacacatt taaaataggg cactactgga 420 acacacagat aggacatcca ggttttgggt caatattgta gactttttgg tggatgagat 480 atgcaggttg atrccagaag gacaacaaaa acatatgtca gatagaaggg aggagcaaat 540 gccaagagct ggagctgagg aagatcactg tgaaattcta tgtagtctag ttggctggat 600 gctagagcaa agaggtgg 618 72 806 DNA Homo sapien 72 tctacgatgg ccatttgctc attgtctttc ctctgtgtgt agtgagtgac cctggcagtg 60 tttgcctgct cagagtggcc cctcagaaca acagggctgg ccttggaaaa accccaaaac 120 aggactgtgg tgacaactct ggtcaggtgt gatttgacat gagggccgga ggcggttgct 180 gacggcagga ctggagaggc tgcgtgcccg gcactggcag cgaggctcgt gtgtccccca 240 ggcagatctg ggcactttcc caacccaggt ttatgccgtc tccagggaag cctcggtgcc 300 agagtggtgg gcagatctga ccatccccac agaccagaaa caaggaattt ctgggattac 360 ccagtccccc ttcaacccag ttgatgtaac cacctcattt tttacaaata cagaatctat 420 tctactcagg ctatgggcct cgtcctcact cagttattgc gagtgttgct gtccgcatgc 480 tccgggcccc acgtggctcc tgtgctctag atcatggtga ctcccccgcc ctgtggttgg 540 aatcgatgcc acggattgca ggccaaattt cagatcgtgt ttccaaacac ccttgctgtg 600 ccctttaatg ggattgaaag cacttttacc acatggagaa atatattttt aatttgtgat 660 gcttttctac aaggtccact atttctgagt ttaatgtgtt tccaacactt aaggagactc 720 taatgaaagc tgatgaattt tcttttctgt ccaaacaagt aaaataaaaa taaaagtcta 780 tttagatgtt gaaaaaaaaa aaaaaa 806 73 301 DNA Homo sapien misc_feature (1)...(301) n = A,T,C or G 73 actctggtaa gcttgttgtt gtccaagtga agctccctca gatgaggcgt gttggccana 60 gagccattgt caacagcaga gatgctgttg aaactcaatc ccaacttagc caaattattc 120 agtcctttca ggctagctgc atcaactctg ctgattttgt tgccatcaag atgtaattcc 180 gtaagggaag gaggaagacc ttgaggaatg ctggygatat tggyatcagc aatgcggatg 240 tasgaagagc ttcttcmttc cctggaaagc cccattttca atyccttgag ctcttcakcg 300 g 301 74 401 DNA Homo sapien 74 agtttacatg atccctgtaa cagccatggt ctcaaactca gatgcttcct ccatctgcca 60 agtgtgttct ggatacagag cacatcgtgg cttctggggt cacactcagc ttaggctgtg 120 ggtccacaga gcactcatct ggctgggcta tggtggtggt ggctctactc aagaagcaaa 180 gcagttacca gcacattcaa acagtgtatt gaacatcttt taaatatcaa agtgagaaac 240 aagaaggcaa cataataatg ttatcagaaa gatgttagga agtaaggaca gctgtgtaaa 300 gcttgaggct gaaaagtagc ttgccagctt catttctttg gtttcttggg tagtgggccg 360 ccggaacagc aagatgtgag gttctggttc atggatcata t 401 75 612 DNA Homo sapien 75 ttatttttca atttttattt tggttttctt acaaaggttg acattttcca taacaggtgt 60 aagagtgttg aaaaaaaaat tcaaattttt ggggagcgag ggaaggagtt aatgaaactg 120 tattgcacaa tgctctgatc aatccttctt tttctctttt gcccacaatt taagcaagta 180 gatgtgcaga agaaatggaa ggattcagct ttcagttaaa aaagaagaag aagaaatggc 240 aaagagaaag ttttttcaaa tttctttctt ttttaattta gattgagttc atttatttga 300 aacagactgg gccaatgtcc acaaagaatt cctggtcagc accaccgatg tccaaaggtg 360 caatatcaag gaagggcagg cgtgatggct tatttgtttt gtattcaatg attgtctttc 420 cccattcatt tgtcttttta gagcagccat ctacaagaac agtgtaagtg aacctgctgt 480 tgccctcagc aacaagttca acatcattag agccctgtag aatgacagcc tttttcaggt 540 tgccagtctc ctcatccatg tatgcaatgc tgttcttgca gtggtaggtg atgttctgag 600 aggcatagtt gg 612 76 844 DNA Homo sapien 76 ggctttcgag cggccgcccg ggcaggtctg atggttctcg taaaaacccc gctagaaact 60 gcagagacct gaaattctgc catcctgaac tcaagagtgg agaatactgg gttgacccta 120 accaaggatg caaattggat gctatcaagg tattctgtaa tatggaaact ggggaaacat 180 gcataagtgc caatcctttg aatgttccac ggaaacactg gtggacagat tctagtgctg 240 agaagaaaca cgtttggttt ggagagtcca tggatggtgg ttttcagttt agctacggca 300 atcctgaact tcctgaagat gtccttgatg tgcagcykgc attccttcga cttctctcca 360 gccgagcttc ccagaacatc acatatcact gcaaaaatag cattgcatac atggatcagg 420 ccagtggaaa tgtaaagaag gccctgaagc tgatggggtc aaatgaaggt gaattcaagg 480 ctgaaggaaa tagcaaattc acctacacag ttctggagga tggttgcacg aaacacactg 540 gggaatggag caaaacagtc tttgaatatc gaacacgcaa tgctgttcct tgacattgca 600 ccaccaatgt ccagaggtgc aatgtcaagg aacggcaggc gagatggctt atttgttttg 660 tattcaatga ttgtcttgcc ccattcattt gtctttttgg agcagccatc gactaggaca 720 gagtaggtga acctgctgtt gccctcagca acaagttcca catcgttgga accctgcaga 780 agcacagcct tgttcaarct gcccgtctcc tcatccagat acctcggccg cgaccacgct 840 aatc 844 77 314 DNA Homo sapien 77 ccagtcctcc acttggcctg atgagagtgg ggagtggcaa gggacgtttc tcctgcaata 60 gacacttaga tttctctctt gtgggaagaa accacctgtc catccactga ctcttctaca 120 ttgatgtgga aattgctgct gctaccacca cctcctgaag aggcttccct gatgccaatg 180 ccagccatcc tggcatcctg gccctcgagc aggctgcggt aagtagcgat ctcctgctcc 240 agccgtgtct ttatgtcaag cagcatcttg tactcctggt tctgagcctc catctcgcat 300 cggagctcac tcag 314 78 548 DNA Homo sapien 78 accaagagcc aagtgttaca caggatattt taaaaataaa atgtttttgg aatcctcacc 60 tcccatgcta tcttctaaga taactacaaa tattcttcaa agatttaact gagttctgcc 120 aaggacctcc caggactcta tccagaatga ttattgtaaa gctttacaaa tcccaccttg 180 gccctagcga taattaggaa atcacaggca aacctcctct ctcggagacc aatgaccagg 240 ccaatcagtc tgcacattgg ttttgttaga tactttgtgg agaaaaacaa aggctcgtga 300 tagtgcagct ctgtgcctac agagagcctc ccttttggtt ctgaaattgc tgatgtgaca 360 gagacaaagc tgctatgggt ctaaaacctt caataaagta actaatgaca ctcaaggtcc 420 tgggactctg agacagacgg tggtaaaacc cacagctgcg attcacattt ccaatttatt 480 ttgagctctt tctgaagctg ttgcttccta cctgagaatt cccatttaga gagctgcaca 540 gcacagtc 548 79 646 DNA Homo sapien 79 accccgtcac tatgtgaata aaggcagcta gaaaatggac tcaattctgc aagccttcat 60 ggcaacagcc catattaaga cttctagaac aagttaaaaa aaatcttcca tttccatcca 120 tgcatgggaa aagggcttta gtatagttta ggatggatgt gtgtataata ataaaatgat 180 aagatatgca tagtggggga ataaagcctc agagtccttc cagtatgggg aatccattgt 240 atcttagaac cgagggattt gtttagattg ttgatctact aatttttttc ttcacttata 300 tttgaatttt caatgatagg acttattgga aattggggat aattctgttg tggtattaaa 360 taatattcat tttttaaaaa ctcatcttgg tattgagtta gtgcattgac ttccaatgaa 420 ttgacataag cccatatttc attttaacca gaaacaaaaa ctagaaaatg ttactcccta 480 aataggcaac aatgtatttt ataagcactg cagagattta gtaaaaaaca tgtatagtta 540 ctttagaaac aacttctgac acttgagggt tacccaatgg tctccttccc attctttata 600 tgaggtaaat gcaaaccagg gagccaccga ataaacagcc ctgagt 646 80 276 DNA Homo sapien misc_feature (1)...(276) n = A,T,C or G 80 gtctgaatga gcttcnctgc gagatgganc ancataaccc agaantccaa aancntanng 60 aacgnnaaaa cccgntngaa caagnaaacn gcaactnacg gccgcctgnt gnagggcgag 120 gacgcccacc tctcctcctc ccagttctcc tctggatcgc agncatccan agatgtgacc 180 tcttccagcc gccaaatccg caccaaggtc atggatgtgc acgatggcaa ggtgggtgtc 240 cacccacgaa caggtccttc gcaccaagaa ctgagg 276 81 647 DNA Homo sapien 81 gtcctgcctt tcatcttttc tttaaaaaaa ataaatgttt acaaaacatt tccctcagat 60 tttaaaattc atggaagtaa taaacagtaa taaaatatgg atactatgaa aactgacaca 120 cagaaaaaca taaccataaa atattgttcc aggatacaga tattaattaa gagtgacttc 180 gttagcaaca cgtagacatt catacatatc cggtggaaga ctggtttctg agatgcgatt 240 gccatccaaa cgcaaatgct tgatcttgga gtaggrtaat ggccccagga tcttgcagaa 300 gctctttatg tcaaacttct caagttgatt gacctccagg taatagtttt caaggttttc 360 attgacagtt ggtatgtttt taagcttgtt ataggacaga tccagctcaa ccagggatga 420 cacattgaaa gaatttccag gtattccact atcagccagt tcgttgtgag ataaacgcag 480 atactgcaat gcattaaaac gcttgaaata ctcatcaggg atgttgctga tcttattgtt 540 gtctaagtag agagttagaa gagagacagg gagaccagaa ggcagtctgg ctatctgatt 600 gaagctcaag tcaaggtatt cgagtgattt aagaccttta aaagcag 647 82 878 DNA Homo sapien 82 ccttctttcc ccactcaatt cttcctgccc tgttattaat taagatatct tcagcttgta 60 gtcagacaca atcagaatya cagaaaaatc ctgcctaagg caaagaaata taagacaaga 120 ctatgatatc aatgaatgtg ggttaagtaa tagatttcca gctaaattgg tctaaaaaag 180 aatattaagt gtggacagac ctatttcaaa ggagcttaat tgatctcact tgttttagtt 240 ctgatccagg gagatcaccc ctctaattat ttctgaactt ggttaataaa agtttataag 300 atttttatga agcagccact gtatgatatt ttaagcaaat atgttattta aaatattgat 360 ccttcccttg gaccaccttc atgttagttg ggtattataa ataagagata caaccatgaa 420 tatattatgt ttatacaaaa tcaatctgaa cacaattcat aaagatttct cttttatacc 480 ttcctcactg gccccctcca cctgcccata gtcaccaaat tctgttttaa atcaatgacc 540 taagatcaac aatgaagtat tttataaatg tatttatgct gctagactgt gggtcaaatg 600 tttccatttt caaattattt agaattctta tgagtttaaa atttgtaaat ttctaaatcc 660 aatcatgtaa aatgaaactg ttgctccatt ggagtagtct cccacctaaa tatcaagatg 720 gctatatgct aaaaagagaa aatatggtca agtctaaaat ggctaattgt cctatgatgc 780 tattatcata gactaatgac atttatcttc aaaacaccaa attgtcttta gaaaaattaa 840 tgtgattaca ggtagagaac ctcggccgcg accacgct 878 83 645 DNA Homo sapien 83 acaaacattt tacaaaaaag aacattacca atatcagtgg cagtaagggc aagctgaaga 60 ataaatagac tgagtttccg ggcaatgtct gtcctcaaag acatccaaac tgcgttcagg 120 cagctgaaac aggcttcttt cccagtgaca agcatatgtg gtcagtaata caaacgatgg 180 taaatgaggc tactacatag gcccagttaa caaactcctc ttctcctcgg gtaggccatg 240 atacaagtgg aactcatcaa ataatttaaa cccaaggcga taacaacgct atttcccatc 300 taaactcatt taagccttca caatgtcgca atggattcag ttacttgcaa acgatcccgg 360 gttgtcatac agatacttgt ttttacacat aacgctgtgc catcccttcc ttcactgccc 420 cagtcaggtt tcctgttgtt ggaccgaaag gggatacatt ttagaaatgc ttccctcaag 480 acagaagtga gaaagaaagg agaccctgag gccaggatct attaaacctg gtgtgtgcgc 540 aaaagggagg gggaaggcag gaatttgaaa ggataaacgt ctcctttgcg ccgaggaatc 600 aggaagcgtg actcacttgg gtctgggacg ataccgaaat ccggt 645 84 301 DNA Homo sapien misc_feature (1)...(301) n = A,T,C or G 84 tctgatgtca atcacaactt gaaggatgcc aatgatgtac caatccaatg tgaaatctct 60 cctcttatct cctatgctgg agaaggatta gaaggttatg tggcagataa agaattccat 120 gcacctctaa tcatcgatga gaatggagtt catgggctgg tgaaaaatgg tatttgaacc 180 agataccaag ttttgtttgc cacgatagga atagctttta tttttgatag accaactgtg 240 aacctacaag acgtcttgga caactgaagn ttaaatatcc acangggttt attttgcttg 300 g 301 85 296 DNA Homo sapien misc_feature (1)...(296) n = A,T,C or G 85 agcgtgggtc gcggcncgan gtagagaacc gactgaaacg tttgagatga agaaagttct 60 cctcctgatc acagccatct tggcagtggc tgttggtttc ccagtctctc aagaccagga 120 acgagaaaaa agaagtatca gtgacagcga tgaattagct tcagggtttt ttgtgttccc 180 ttacccatat ccatttcgcc cacttccacc aattccattt ccaagatttc catggtttan 240 acgtaatttt cctattccaa tacctgaatc tgcccctaca actccccttc ctagcg 296 86 806 DNA Homo sapien 86 tctacgatgg ccatttgctc attgtctttc ctctgtgtgt agtgagtgac cctggcagtg 60 tttgcctgct cagagtggcc cctcagaaca acagggctgg ccttggaaaa accccaaaac 120 aggactgtgg tgacaactct ggtcaggtgt gatttgacat gagggccgga ggcggttgct 180 gacggcagga ctggagaggc tgcgtgcccg gcactggcag cgaggctcgt gtgtccccca 240 ggcagatctg ggcactttcc caacccaggt ttatgccgtc tccagggaag cctcggtgcc 300 agagtggtgg gcagatctga ccatccccac agaccagaaa caaggaattt ctgggattac 360 ccagtccccc ttcaacccag ttgatgtaac cacctcattt tttacaaata cagaatctat 420 tctactcagg ctatgggcct cgtcctcact cagttattgc gagtgttgct gtccgcatgc 480 tccgggcccc acgtggctcc tgtgctctag atcatggtga ctcccccgcc ctgtggttgg 540 aatcgatgcc acggattgca ggccaaattt cagatcgtgt ttccaaacac ccttgctgtg 600 ccctttaatg ggattgaaag cacttttacc acatggagaa atatattttt aatttgtgat 660 gcttttctac aaggtccact atttctgagt ttaatgtgtt tccaacactt aaggagactc 720 taatgaaagc tgatgaattt tcttttctgt ccaaacaagt aaaataaaaa taaaagtcta 780 tttagatgtt gaaaaaaaaa aaaaaa 806 87 620 DNA Homo sapien 87 tttttgcatc agatctgaaa tgtctgagag taatagtttc tgttgaattt ttttttgttc 60 atttttctgc acagtccatt ctgtttttat tactatctag gcttgaaata tatagtttga 120 aattatgaca tccttcctct ttgttatttt cctcatgatt gctttggcta ttcaaagttt 180 attttagttt catgtaaatt tttgaattgt attttccatt attgtgaaaa tagtaccact 240 gcaattttaa taggaagttt attgaatcta tagattactt tggataatat ggcacttcaa 300 taatattcat gttttcaatt catagacaaa atattttaaa atttatttgt atcttttcta 360 atttttcctt tttttattgt aaagatttac ctccttggtt aatattttcc tcagaaattt 420 attatttaag gtatagtcaa taaaattttc ttcctctatt ttgtcagata gtttaagtgt 480 atgaaaccat agatatactt gtatgttaat tttatatttt gctaatttac tgagtgtatt 540 tattagttta gagaggtttt aatgtactgt ttatggtttt ttaaatataa gattacttat 600 tttttaaaaa aaaaaaaaaa 620 88 308 DNA Homo sapien misc_feature (1)...(308) n = A,T,C or G 88 tagctgtgnt cagcaggccg aggttttttt tttttttgag atggagtctc gccctgtcac 60 ccaggctgga gtgcagtggc ctgatctcag ctcactgcaa gctccacctc ctggattcac 120 gctattctcc tgcctcagcc tcccaagtag ctgggactac aggcgcccgc caccacgccc 180 agctaattnt ttgnattttt agtacnagat gcggtttcat cgtgttagcc agcatggnct 240 cgatctcctg acctcgtgaa ctgcccgcct cggcctccca aagacctgcc cgggcnggcc 300 gctcgaaa 308 89 492 DNA Homo sapien misc_feature (1)...(492) n = A,T,C or G 89 agcggccgcc cgggcaggtc tgttaagtaa catacatatc accttaataa aaatcaagat 60 gaaatgtttt agaaactatt ttatcaaaag tggctctgat acaaagactt gtacatgatt 120 gttcacagca gcactattaa tgccaaaaag tagacaaaac ctaaatgtcc attaactgat 180 aagcaaaatg tggtatatcc atacaatgga atattatgta gcccacaaca tggcatggag 240 tactacaaca tggatgagcc tcaaaaacgt tatgctaaat gaaaaaagtc agatatagga 300 aaccacatgt catatgatcc catttatatg aaatagccag aaaaggcaag tcatagaaac 360 aagatagatc ggaaaatggg ttggaggact acaaatggca ccagggatct ttgaagttga 420 tggaaatggt ctaaaatcag actgtggntg tggttgaaca agtctgtaaa tttaccaaaa 480 tgcgttaata ca 492 90 390 DNA Homo sapien misc_feature (1)...(390) n = A,T,C or G 90 tcgagcggcc gcccgggcag gtacaagctt tttttttttt tttttttttt ttttctaaca 60 gttctctgtt ttattgcaat acagcaaagt ctggttaata ttaagngata tcaacataaa 120 gtattggtga ggagtctttt gtgacatttt ttaccatccc accttaaata tttctgtgca 180 aaanaatcca catcattgtt tggtancana ggatctctta aaaagttccc taanacactg 240 agggcataaa accaaacaaa ataaaataag gagtgatagg ctaaagcagt atcttcccct 300 ccatccacat ttgncaagca ttatattcta accaaaaaat gatcacacca ggccatgcaa 360 aactgtccaa tattaccgag aaaaaaccct 390 91 192 DNA Homo sapien 91 agcgtggtcg cggccgaggt ctgtcaatta atgctagtcc tcaggattta aaaaataatc 60 ttaactcaaa gtccaatgca aaaacattaa gttggtaatt actcttgatc ttgaattact 120 tccgttacga aagtccttca catttttcaa actaagctac tatatttaag gcctgcccgg 180 gcggccgctc ga 192 92 570 DNA Homo sapien misc_feature (1)...(570) n = A,T,C or G 92 agcgtggtcg cggccgaggt ctgacaacta acaaagaagc aaaaactggc atcttggaca 60 tcctagtatt acacttgcaa gcaattagaa cacaaggagg gccaaggaaa aagtttagct 120 ttgaatcact tccaaatcta ctgattttga ggttccgcag tagttctaac aaaacttttc 180 agacaatgtt aactttcgat taagaaagaa aaaaacccca aacatcttca ggaattccat 240 gccaggttca gtctcttcca gtgagcccgc ttgctaaaag tccacgtgca ccattaatta 300 gctgggctgg cagcaccatg taaaaagaag cctattcacc accaaccaca cagactagac 360 atgtaaagta ggatcaagta atggatgaca accatggtcg tggaatatgg tcaatgagag 420 tcagaaaagt acaggcacca gtacaagcag cagataacag aattgacggg ccaaaggata 480 aaaataggct tatttaaata ggatgctaca gaacacatnc acttctaatt ggaagctgct 540 ttacactggg tggcattgna ccatatgcat 570 93 446 DNA Homo sapien misc_feature (1)...(446) n = A,T,C or G 93 tcgagcggcc gcccgggcag gtccaggttt ttatttagtt gtgtaatctt ggacaagtta 60 cctaactttt ttgagtctga atatatttaa tctgcaaaat gagaatcatg ataatacgtc 120 ataggcttaa ttaggaggat taaatgaaat aatttatagg tggtgccatg gttacataca 180 agtattagta gttaattctt ttcctttgtt tacttttata gtataggttg gatgaaggtt 240 ccagtatagg caaaaatact acttgggggt aaagtagagt gtgatacttt atttgaaatg 300 ttccctgaat ctgatcttta ctttttgnta ctgctgcact acccaaatcc aaattttcat 360 cccaacattc ttggatttgt gggacagcng tagcagcttt tccaatataa tctatactac 420 atcttttctt actttggtgc tttttg 446 94 409 DNA Homo sapien 94 cgagcggccg cccgggcagg tccatcagct cttctgctta gaatacgagg cagacagtgg 60 agaggtcaca tcagttatcg tctatcaggg tgatgaccca agaaaggtga gtgagaaggt 120 gtcggcacac acgcctctgg atccacccat gcgagaagcc ctcaagttgc gtatccagga 180 ggagattgca aagcgccaga gccaacactg accatgttga aggcgttctc tccaggctgg 240 attcactgca ctcggaagaa ttctgcccag ggaatttagt gtgggggtac caggaccagt 300 ttgtcttgat cttgagaccc ccagagctgc tgcatccata gggtgttgca ggactacacc 360 tggcctgcct tgcagtcatt ctttcttata tgttgaccca tttgcccaa 409 95 490 DNA Homo sapien misc_feature (1)...(490) n = A,T,C or G 95 tcgagcggcc gcccgggcag gtcctacttg tttgcagctt ccacacactg cacctaccta 60 ctacctctct tccatgctta actgggttta gaaaggtgag ctatgcgtag aagaactact 120 tgggatattc aagtgctgta tttgaacgat aagcctatag ataacagtct gaagctgcaa 180 gggagacttt gttagtacac tactataaac aggtaaacta cctgtttgta cttgatatag 240 tgcatatgaa atgactgatt taatacaaaa ctacagaaca tgcaaaattt tttctgagat 300 gttaagtatt acttcagtgg agaacaaaac ttacttaacc tttcgctaat gcatgtagta 360 ccagaaagca aacatggttt tagcttcctt tactcaaaat atgaacatta agtggttgtg 420 aattttgtct gccaagtggt tcagaaaata cattataaat aacctaagtt aaaaaaaaga 480 aactgngaac 490 96 223 DNA Homo sapien 96 agcgtggtcg cggccgaggt ctggaagccc accctaggac ttgaatggca ccttgtcctt 60 tctctgccag taatgcaatc caacacaata tgctacaggg aaaacagaat ttccacggtg 120 ccgccctctg gtacaaggga aacagcacgc aaagcaaaag gccacagagg gctccctgag 180 aatccagtac aactaagcga ggacctgccc gggcggccgc tcg 223 97 527 DNA Homo sapien misc_feature (1)...(527) n = A,T,C or G 97 tcgagcggcc gcccgggcag gtctgtgcag gagacactga agtgggtagt gtccataatc 60 tttttagcct gttgctgaaa ttccagttgt actccttcaa accaaaatgc ttacaggatc 120 atgggaaagc ctcggttgca gaaatcaaga caggcaagtg ggaagataac tcggctttga 180 ggttaaacag atctgggttc aaagcatagt ttcactctct gtcttgtgaa gtgtcctggg 240 tgaagtcatt tcctctcttg aatttcagag aggatgaaaa tataaaaagt ataataacta 300 tcttcataat ctttgtgagg attaaagaag acgaagtgtg tgaaaagcta agcacagagc 360 aggcattcta caataagtag ttattatttt tggaaccatc ccgnccctag ccccagccca 420 attaccttct cttagnctct tcatatcgaa ngccgtaatc ttgaccttct cttgcnactg 480 gattggtgct ggttgatgcc caaacttccc gagatgctgt ctgggaa 527 98 514 DNA Homo sapien misc_feature (1)...(514) n = A,T,C or G 98 tcgagcggcc gcccgggcag gtctggctcc catggccctt ggggtggcct gactctgtca 60 ctattcctaa aaccttctag gacatctgct ccaggaagaa ctttcaacac caaaattcat 120 ctcaatttta cagatgggaa aagtgattct gagaccagac cagggtcagg ccaaggtcat 180 ccagcatcag tggctgggct gagactgggc ccagggaacc ctgtctgctc ctctttttcc 240 cagagctgtg agttctctag ccaaggctgc actcttgagg gagagccagg aagcatagct 300 gaggccatga caacctcact cttcacctga aaatttaacc cgtggcagag gatccaggca 360 catataggct tcggagccaa acaggacctc ggccgcgacc acgctaagcc gaattccagc 420 acactggcgg ccgttactag tggatcccga gcttnggtac caagcttggc gtaatcatgg 480 gcatagctgg ttcctggggt gaaaatggta tccg 514 99 530 DNA Homo sapien misc_feature (1)...(530) n = A,T,C or G 99 tcgagcggcc gcccgggcag gtctgaagaa acaggtataa atttggcagc cagtaatttt 60 gacagggaag ttacagcttg catgacttta aatatgtaaa tttgaaaata ctgaatttcg 120 agtaatcatt gtgctttgtg ttgatctgaa aaatataaca ctggctgtcg aagaagcatg 180 ttcaaaaata tttaattcac ttcaaaatgt catacaaatt atggtggttt ctatgcaccc 240 ctaaagcttc aagtcattta gctcaggtac atactaaagt aatatattaa ttcttccagt 300 acagtggtgt ttcataccat tgacatttgc ataccctaga ataatttaag aaagacatgt 360 gtaatattca caatgttcag aaaagcaagc aaaaggtcaa ggaacctgct ttggttcttc 420 tggagatggn ctcatatcag cttcataaac attcattcta caaaatagta agctaaccat 480 ttgaacccca atttccagat taagcatatt ttctcataaa tnatgaagcc 530 100 529 DNA Homo sapien 100 agcgtggtcg cggccgaggt ccaggcacgg tggcttatgt gtgtaatccc agcacttggg 60 gaggctgagg gaggtggatc acttgagtcc aggagtttga gaccagtctg ggcaacatgg 120 cgaaacttca tcactaccaa agaagaaaaa aattagccag gtgtggtggt gtatgcctgt 180 agtcccagat actctggtgg ctgaggtgag aggatagctt gagcccagga aattgaggct 240 gcagtgaact atgattgcac tactgtgctc cagcttgggc aacagagtga gatcttgtct 300 ccaaaagtcc ttgaaggatt ttaggaagtt gttaaaagtc ttgaaacgat gtttgggggc 360 atgttagggt tcttgaatgt ttaattcctc taataactgc ttattcaaga gaagcatttc 420 tgactgggtg cggggcagtg gcttcatgcc ccataatccc agtactttgg gaggctgaag 480 caggaacatt gcttgagccc aggacttcaa gaacagcctg ggtaacata 529 101 277 DNA Homo sapien 101 tcgagcggcc gcccgggcag gtcgcaggaa gaggatggaa actgaggagt ccaggaagaa 60 gagggaacga gatcttgagc tggaaatggg agatgattat attttggatc ttcagaagta 120 ctgggattta atgaatttgt ctgaaaaaca tgataagata ccagaaatct gggaaggcca 180 taatatagct gattatattg atccagccat catgaagaaa ttggaagaat tagaaaaaga 240 agaagagctg agaacagacc tcggccgcga ccacgct 277 102 490 DNA Homo sapien 102 gcgtggtcgc ggccgaggtc tgacggcttt gctgtcccag agccgcctaa acgcaagaaa 60 agtcgatggg acagttagag gggatgtgct aaagcgtgaa atcagttgtc cttaattttt 120 agaaagattt tggtaactag gtgtctcagg gctgggttgg ggtccaaagt gtaaggaccc 180 cctgccctta gtggagagct ggagcttgga gacattaccc cttcatcaga aggaattttc 240 ggatgttttc ttgggaagct gttttggtcc ttggaagcag tgagagctgg gaagcttctt 300 ttggctctag gtgagttgtc atgtgggtaa gttgaggtta tcttgggata aagggtcttc 360 tagggcacaa aactcactct aggtttatat tgtatgtagc ttatattttt tactaaggtg 420 tcaccttata agcatctata aattgacttc tttttcttag ttgtatgacc tgccccgggc 480 ggccgctcga 490 103 490 DNA Homo sapien 103 gagcggccgc ccgggcaggt ccaaaccagc ttgctcataa gtcattaacc aaatccatta 60 taggtaattt gttcagttca atgtttacaa ttcttatgga aaaaattagc aacacacaca 120 tttaaaacgt gtgcatttac ctttgcgtga gtgcttaaaa tacatatttc tatttcaaga 180 tgacatttaa aaattattct aatatatcag cagcaaaaat ataatttgca attacaaaaa 240 actaaactag aatccttaag ttattctcat gtttacagtt gtgattcttt aataaatact 300 attatgcagc tctattgttt aagctttctg gatttggttt aaacacatgc atatatattg 360 tcaattgtgg gaagctttac aagttatatt ccatgcactt tttggacaga gttctaacag 420 agccagccag tccacaaaac aggcaagaca aaagttgaat taactggggc aaaataggac 480 tcttatgcaa 490 104 489 DNA Homo sapien 104 cgtggtcgcg gccgaggtcc aggctggtct cgaactcctg accttgtgat ctgcccgcct 60 cggcctccca aagtgttggg attacaggca tgagccactg cgcccgaccg agttgaacat 120 ttaatgtcag actaggccag agtttctcaa tctttttatt ctcacttccc aaaggagccg 180 ttggagattt tcccctcaat ctctctcctt catgaaattt cataccacaa atatagtatg 240 ttttatttat gtactgtgac cctttgaagg atcacaaacc aatataatag tttttctttt 300 taacccgtca aggaccaagt ttttgcccct gttggaaatg cataaactgg actgatgaat 360 tggtatagat ggcttttatc atgaggatca gaaaaacttg aaattccttg gctacgacac 420 tccatattta tcaccgtata gggaggacct tggtatgggg aagtagaaac acttctacac 480 tttacagca 489 105 479 DNA Homo sapien misc_feature (1)...(479) n = A,T,C or G 105 gcgtggtcgc ggccgaggtc tgactggctt cagccccaga agttgagctg gcctttagac 60 aaaataattg cacctccctc tgctgcttat tcccttccgt ttttcatttg agtgtgaaca 120 gttagataaa atctgtggct gnctcttcca ccttgctcta gtttccattg ctgtgagcag 180 gccctcctat gccccgcatt tagctacaat gctgtggact cacttgattc tttttctccg 240 agctttgtct agaaatatgt gaaggtgagg ttaagtgctt ctctgtgtag atccacttag 300 ccctgtctgc tgtctcgatg ggcgttgctt cgtctctcct ctcttccatc ctttccattt 360 gcttctcacc accttctggc ttcttttctt aatgcaataa aggcagtttc taacaaagaa 420 agaatgtggg ctttggagtt agacagacct ggntttaaat tctgcttctg gctctccaa 479 106 511 DNA Homo sapien 106 tcgcggccga ggtccaaaac gtggattcca atgacctgcc ttgagcccgc ggttgccagg 60 agttggacct gcagtagtat gggaagctca cggcctaaat accgactgcc ctctgacccc 120 accgtccagc gattctagaa catttctagt aggaaagaca tagcaaggga ttttcatgat 180 tgggaaatac tgggagacaa gctgaagatt tgttaagggc tatgcttctg tcatctttta 240 ggtatttaag gctactcctt tagctagcta ctttgagctg tttaaagtga ctatctccct 300 acacagagtt acacaatgag catctctgaa agagaatatt accctggatt tccaaagatg 360 tactctaaca ggatgaccag gcaaaaggtg acccggggga ggagtctgtt ataacactcg 420 gacccacatg ttctcaaggc acttcagaac tttgggaaat cattttgtac cggatcctca 480 gaaagcattt atggaaatac acatccttta g 511 107 451 DNA Homo sapien 107 ggccgcccgg gcaggtccag aatatcaaat caaaaggtca caaatgttca cttcctcctc 60 caccctctta catattggat cttcaattgc aatagggagt gtaagatggg cattttagag 120 acgtagttgc atcagcagaa gcaaacccat cttatacaaa tgggttttgg ggataggaaa 180 aggctgctaa aaattcacaa gtcaccattc cccagaagca atgaatagcc gtagaagacc 240 aaggaagatc aacaagtttc caaagtgcta aagccagaga tttggccctt ccaaaatacc 300 accaggacgc ctggacccgt gggctctccg catgtcacca ctgactgcca ggatgctgct 360 gcacctccct tccttgagac acaacagaga gacagtgaag tcacccaaga ctgggatcat 420 cagaggctcc tcatgcttgc tacagagaag c 451 108 461 DNA Homo sapien 108 ccgcccgggc aggtcctgaa aacattcaga ctaatcaaaa tggtactact gtaacttctt 60 ataatacata atataaaagt ttttgaaaga tatagacaca attaacccct aaacaacaca 120 ctatctgatt ctcaaaagca atggctattt aacaagatgt aaaaggacaa taacatatca 180 aagaactttc acacacctaa agatagcatt tagcagcaag ttagtcagac aaaacaaaca 240 caaatatttt cacatttcct atgtttgttt ttaactttac ttcataaagc cactgataat 300 tgaggtttct ttcaagtata agatttctaa aattaaaaac tgtttttgac atatttttat 360 aaagaaataa aaagcaaaac gcaatccaac tatttatatg agtccctctt ctccaacagc 420 tttagatggt tttctgagta cttttttaca cagaatattt t 461 109 441 DNA Homo sapien 109 ggccgcccgg gcaggtctga ttataagaga aagaaatcca gtgacacgag ggcaggcagg 60 ccccgctctg ctctgatcga gaaaagcttc ctgatgtcag ggagatggaa ctgccaccat 120 cagaaccatg gcactttggg tgaaggtgtg tcagcgacca agggggcagg aaatgggcag 180 tgactaaggg ggcaggaaac aggcaggcac atggcaaggt tctcccagcc catcagccca 240 gtgatggcct cgattttgaa gctgcactac tgtctgaaaa gcacaattac tggtgactct 300 taacaaactt cagcatactg gggaaggaga ctgtcaagta actgaattgg aaagatgaaa 360 aagaaccatc tctaaaagtt gatgcttgtc agaagaataa cctcctttgt gcaagtcttg 420 caacatcttc attcaaccac a 441 110 451 DNA Homo sapien misc_feature (1)...(451) n = A,T,C or G 110 ggtcgcggcc gaggtctggg gaaggggtga gaatccctgg gccttgccca gtcctgagct 60 ctgggtgtct gcagggaagc acagtggtga gttagtgtta aagaaagcat ccagagaggt 120 aagaggggct tgggtagcac cctttgcctc tgtcacttcc gcaaaaactt cttgttgagg 180 aggaagatga gaaggttgac attgactttg gccttgttga agagtttcat gacagccaca 240 ccctcatact ggagctgcan gagatcctga tagtgaagct tgaaatcgct ccatgtccac 300 acccaggaac ttggcattta cttcaaactt tcctgcctca tctcccggcg tgatgtcaaa 360 natgacgttt cttgaagtga gaggcgggaa agatcttcaa tttccaccaa agacaccctt 420 tttccaggaa gcttgagcaa caagtgtaat g 451 111 407 DNA Homo sapien misc_feature (1)...(407) n = A,T,C or G 111 ggccgacgtt cgacctgact tctttngagc agntgncact acccgtcttg aggaatgccg 60 actgcagaca gtggcccang gcaaagagtg tgcgtcatcg atganattgg naagatggag 120 ctcttcagtc agnttttcat tcaagctgnt cgtcagacgc tgtctacccc agggactata 180 atcctnggca caatcccagt tcctanagga aagccactgn ctcttgtaga agaaatcana 240 cacanaaagg atgtgaacng tgtttaatgt caccaaggga aaacatgaaa ccaccttctg 300 ccagatatcg ggacgttgcg tgcagatcaa gcacgnaagt gaagacgcgt gcattccttg 360 ccttccgtga acgantgccc agntcaagaa gancctgatg gaaccct 407 112 401 DNA Homo sapien misc_feature (1)...(401) n = A,T,C or G 112 tcgcggccga ggtcggccga ggtctgacat ctgttgtctg tgataaccac ttctgtattg 60 cgtcttaacc acttctgtat tgtgtggttt taactgccta aggcggcaat gggcagtggg 120 cccctttccc ttaggatggg tatcaattca acaatattta taaggcattt actgtgtgct 180 aagcatttgg aagacccagg ctacaaaata agacatagtt cctgccctcc aggccagcag 240 agggaggcac aaatacccag gaatctctga tgggtgtgaa gtgcggtcgt gggccacaga 300 aaatgaccgt catggagacc ctgctaaagg tcggaccctg agcccaaagg ggtattcaga 360 agnggagatg attttggccc cactcataga tgggtggcaa a 401 113 451 DNA Homo sapien 113 gtcgcggccg aggtccatat taaaaagtcc atcataaaca aagactcctc ctcatggtat 60 gaatatgctc catatgccca taatggtgca taacggactt agaaattcca atgagtctta 120 gggttgaaat ttccaatgac ctgagcaagg cagctcccta tagcttctgg ataacatttt 180 acacccagag ttcaggctta aacagaccta tcaacacaat tattttcgga ttgtctgtct 240 agaaaacggc aatgctcaaa ggaatataaa taagggtggg gggacatatg cttccagcct 300 ggcctttctc catgtggtaa aaaacaatgg aatggctgtg ttaatttttt tttaatcttt 360 tctgaccttt actatgtttg gtaatggaaa taagtcaggg aaaacaaaat gaacaggtct 420 catcacttaa ttaatactgg gttttcttct t 451 114 441 DNA Homo sapien 114 ggccgcccgg gcaggtccat cctgtcagag atgggagaag tcacagacgg aatgatggat 60 acaaagatgg ttcactttct tacacactat gctgacaaga ttgaatctgt tcatttttca 120 gaccagttct ctggtccaaa aattatgcaa gaggaaggtc agcctttaaa gctacctgac 180 actaagagga cactgttgtt tacatttaat gtgcctggct caggtaacac ttacccaaag 240 gatatggagg cactgctacc cctgatgaac atggtgattt attctattga taaagccaaa 300 aagttccgac tcaacagaga aggcaaacaa aaagcagata agaaccgtgc ccgagtagaa 360 gagaacttct tgaaacttga cacatgtgca aagacaggaa gcagcacagt ctcggcggga 420 ggaagaaaaa aagaacagag a 441 115 431 DNA Homo sapien misc_feature (1)...(431) n = A,T,C or G 115 gccgcccggg caggtccatt ggcggtgaca aaaggaaaag aagcaaagag actcagtcca 60 taatgctgat tagttagaag aaagggctag gattgagaaa gtaccaggaa cttttaatta 120 tttaaaagag aatgctgact gttaatgttt taaatcttac tgttcaaatg tactaatatg 180 aatttttacc ctttgtgcat gaatattcta aacaactaga agacctccac aatttagcag 240 ttatgaaagt taaacttttt attataaaaa ttctaaacct tactgctcct ttaccaggaa 300 catgacacac tatttancat cagttgcata cctcgccaat agtataattc aactgtcttg 360 cccgaacaat catctccatc tggaagacgt aagcctttag aaacacattt ttctattaat 420 ttctctagaa c 431 116 421 DNA Homo sapien 116 gtcgcggccg aggtccagaa atgaagaaga agtttgcaga tgtatttgca aagaagacga 60 aggcagagtg gtgtcaaatc tttgacggca cagatgcctg tgtgactccg gttctgactt 120 ttgaggaggt tgttcatcat gatcacaaca aggaaccggg gctcgtttat caccagtgag 180 gagcaggacg tgagcccccg ccctgcacct ctgctgttaa acaccccagc catcccttct 240 ttcaaaaggg atcctttcat aggagaacac actgaggaga tacttgaaga atttggattc 300 agcccgcgaa gagatttatc aagcttaact cagataaaat cattgaaagt aataaggtaa 360 aagctaagtc tctaacttcc aggcccacgg ctcaagtgaa tttcgaatac tgcatttaca 420 g 421 117 489 DNA Homo sapien 117 agcgtggtcg cggccgaggt aaggctgcga ggttgtggtg tctgggaaac tccgaggaca 60 gagggctaaa tccatgaagt ttgtggatgg cctgatgatc cacagcggag accctgttaa 120 ctactacgtt gacactgctg tgcgccacgt gttgctcaga cagggtgtgc tgggcatcaa 180 ggtgaagatc atgctgccct gggacccaac tggtaagatt ggccctaaga agcccctgcc 240 tgaccacgtg agcattgtgg aacccaaaga tgagatactg cccaccaccc ccatctcaga 300 acagaagggt gggaagccag agccgcctgc catgccccag ccagtcccca cagcataaca 360 gggtctcctt ggcagacctg cccgggcggc cgctcgaaag cccgaattcc agcacactgg 420 cggccgttac tagtggatcc cagctcggta ccaagcttgg cgtaatcatg gtcatagctg 480 gtttcctgt 489 118 489 DNA Homo sapien 118 tcgagcggcc gcccgggcag gtattgaata cagcaaaatt ctatatacaa agtgacctgg 60 acctgctgct tcaaaacatg atcctttctt actaatatct tgatagtcgg tccatagagc 120 attagaaagc aattgactct taaataaaca gaaaagtgcc taatgcacat taaatgaatg 180 gcctaactac tggaacttta gtagttctat aaggtgatta acataggtag gatccagttc 240 ctatgacagg ctgctgaaga acagatatga gcatcaagag gccattttgt gcactgccac 300 cgtgatgcca tcgtgtttct ggatcataat gttcccatta tctgattcta gacacaccac 360 aggaatatca gtggggtcag aggttagctt agctgcttgc tgggctagaa cagatatcac 420 tccagcatgc tcatctgaca gggtcccgcg gcaacccaga ttaagtcctt gtgaatctgt 480 gcacaggga 489 119 181 DNA Homo sapien 119 taggttccag agacttttgg cccaggagga atatttactt ttagctctgg acatcattac 60 aaaaaggaat atttcccaaa cctcttcaga ccgagaatac atgggtaaaa ttattaaata 120 gttgtataat aaaaataatt ttttccttaa aaaaaaaaaa aacctcggcc gcgaccacgc 180 t 181 120 489 DNA Homo sapien misc_feature (1)...(489) n = A,T,C or G 120 gcgtggtcgc ggccgaggtc catttaaaac aaagaaaaat actaaagcca ctagtaaaca 60 tctgatgtgc aaaatacaac atcctctagt tggctttatg ccattattac ataagctcca 120 aatagctcat cttaaattaa aaagaaaaag tggctgtccc atctctgctg cataaatcag 180 attttttttt aaaggtttag agtactttaa ggaagggaag ttcaaaactg ccagtgaaat 240 tcacagagaa tacaaattta gcaatttaat ttcccaaagc tctttgaaga agcaagagag 300 tctctcttct taatgcagtg ttctcccaag aggaactgta attttgcttg gtacttatgc 360 tgggagatat gcaaaatgtg tttttcaatg tttgctagaa tataatggtt cctcttcagt 420 gnctggttca tcctggaact catgggttaa gaaggacttc ttggagccga actgcccggg 480 cgggccntt 489 121 531 DNA Homo sapien 121 cgagcggccg cccgggcagg tggccagcgc tggtcccgca gacgccgaga tggaggaaat 60 atttgatgat gcgtcacctg gaaagcaaaa ggaaatccaa gaaccagatc ctacctatga 120 agaaaaaatg caaactgacc gggcaaatag attcgagtat ttattaaagc agacagaact 180 ttttgcacat ttcattcaac ctgctgctca gaagactcca acttcacctt tgaagatgaa 240 accagggcgc ccacgaataa aaaaagatga gaagcagaac ttactatccg ttggcgatta 300 ccgacaccgt agaacagagc aagaggagga tgaagagcta ttaacagaaa gctccaaagc 360 aaccaatgtt tgcactcgat ttgaagactc tccatcgtat gtaaaatggg gtaaactgag 420 agattatcag gtcccgagga ttaaactggc tcatttcttt gtatgagaat ggcatcaatg 480 gtatccttgc agatgaaatg ggcctaggaa agactcttca acaatttctc t 531 122 174 DNA Homo sapien 122 tcgagcggcc gcccgggcag gtctgccaac agcagaggcg gggcctccgg catcttcaaa 60 gcacctctga gcaggctcca gccctctggc tgcgggaggg gtctggggtc tcctctgagc 120 tcggcagcaa agcagatgtt atttctctcc cgcgacctcg gccgcgacca cgct 174 123 531 DNA Homo sapien misc_feature (1)...(531) n = A,T,C or G 123 agcgtggtcg cggccgaggt cctcaaccaa gagggttgat ggcctccagt caagaaactg 60 tggctcatgc cagcagagct ctctcctcgt ccagcaggcg ccatgcaagg gcaggctaaa 120 agacctccag tgcatcaaca tccatctagc anagagaaaa ggggcactga agcagctatg 180 tctgccaggg gctaggggct cccttgcaga cagcaatgct acaataaagg acacagaaat 240 gggggaggtg ggggaagccc tatttttata acaaagtcaa acagatctgt gccgttcatt 300 cccccagaca cacaagtaga aaaaaaccaa tgcttgtggt ttctgccaag atggaatatt 360 cctccttcct aanttccaca catggccgtt tgcaatgctc gacagcattg cactgggctg 420 cttgtctctg tggtctgggc accagtagct tgggccccat atacacttct cagttcccac 480 anggcttatg gccnangggc angctccaat tttcaagcac cacgaaggaa g 531 124 416 DNA Homo sapien 124 tcgagcggcc gcccgggcag gtccatctat actttctaga gcagtaaatc tcataaattc 60 acttaccaag cccaggaata atgactttta aagccttgaa tatcaactaa gacaaattat 120 gccaattctg atttctcaca tatacttaga ttacacaaag ataaagcttt agatgtgatc 180 attgtttaat gtagacttat ctttaaagtt tttaattaaa aactacagaa gggagtaaac 240 agcaagccaa atgatttaac caaatgattt aagagtaaaa ctcactcaga aagcattata 300 cgtaactaaa tatacatgag catgattata tacatacatg aaactgcaat tttatggcat 360 tctaagtaac tcatttaagt acatttttgg catttaaaca aagatcaaat caagct 416 125 199 DNA Homo sapien misc_feature (1)...(199) n = A,T,C or G 125 agcgtggtcg cggccgaggt gctttttttt tttttttttt tttttttttt gctattctaa 60 aggggaaggc ccctttttat taaacttgta cattttactt tccttctttc anaatgctaa 120 taaaaaactt ttgtttatac ttaaaaaaac cataaatcan acaaacaaaa gaaacgattc 180 caacatcact tctgngatg 199 126 490 DNA Homo sapien 126 cgtggtcgcg gccgaggtcc agttgctcta agtggattgg atatggttgg agtggcacag 60 actggatctg ggaaaacatt gtcttatttg cttcctgcca ttgtccacat caatcatcag 120 ccattcctag agagaggcga tgggcctatt tgtttggtgc tggcaccaac tcgggaactg 180 gcccaacagg tgcagcaagt agctgctgaa tattgtagag catgtcgctt gaagtctact 240 tgtatctacg gtggtgctcc taagggacca caaatacgtg atttggagag aggtgtggaa 300 atctgtattg caacacctgg aagactgatt gactttttag agtgtggaaa aaccaatctg 360 agaagaacaa cctaccttgt ccttgatgaa gcagatagaa tgcttgatat gggctttgaa 420 ccccaaataa ggaagattgt ggatcaaata agacctgata ggcaaactct aatgtggagt 480 gcgacttggc 490 127 490 DNA Homo sapien 127 cgtggtcgcg gccgaggtcg gccgaggtct ggagatctga gaacgggcag actgcctcct 60 caagtgggtc cctgacccct gacccccgag cagcctaact gggaggcacc ccccagcagg 120 ggcacactga cacctcacac ggcagggtat tccaacagac ctgaagctga gggtcctgtc 180 tgttagaagg aaaactaaca agcagaaagg acagccacat caaaaaccca tctgtacatc 240 accatcatca aagaccaaaa gtaaataaaa ccacaaagat gggaaaaaaa cagaacagaa 300 aaactggaaa ctctaaaaag cagagcacct ctcctcttcc aaaggaacgc agttcctcac 360 cagcaatgga acaaagctgg atggagaatg actttgacga gctgagaaaa gaacgcttca 420 gacgatcaaa ttactctgag ctacgggagg acattcaaac caaaggcaaa gaagttgaaa 480 actttgaaaa 490 128 469 DNA Homo sapien misc_feature (1)...(469) n = A,T,C or G 128 cgtggtcgcg gccgaggtgc tttttttttt tttttttttt tttttttttt tgctgattta 60 ttttttctnt ttattgttac atacaatgta taaacacata aaacanaaaa cagtagggat 120 cctctaggat ctctagggan acagtaaagt anaaagaggt ctcanaaaca tttttttaaa 180 gtacaagaca ttcagngctc ggcccaaagg cgtaaaaggt ttanagccag canatagctg 240 nactaaaggc tccgtctntn tccccanagc caggacaacc ccagggagct ntccattagc 300 agccagtcca cgcaggcagg atgctgcgga aaaagctcta tgctganaac attccccttg 360 atggaaagaa gggcaacaca aaaggggtaa ctaanagctc cttcctctcg tgagggcgac 420 aactgaggaa cagaaaagga gtgtcccatg tcacttttga ccccctccc 469 129 419 DNA Homo sapien 129 gcgtggtcgc ggccgaggtc tgattttcat ttaaatattt cagagctata gcatttgcct 60 ccatgctcaa atccacacca ttggggctta agccgctcat gccaacatta gcaaatgaca 120 tgcagtttaa tccagagatc actgcttctg ggctgatgca tgccaacaca ctggcgtgat 180 ccacgttatg tgcatttttc ttcactttag tgggagaatc aatttttact ccaaggcttc 240 ttagttgctt aagagttgca ttaaggacac aatctttgtc caccagtctt gaatgatgtg 300 tttttttctt tgtatggtaa acgttttggg ttctggtgca ttcatgactg ataattactg 360 ctttggtaga cggctgctca agtttccttg gaggaactat ttaataggtg ggttacttg 419 130 354 DNA Homo sapien 130 agcgtggtcg cggccgaggt ccatctgagg agataaccac atcactaaca aagtgggagt 60 gaccccgcag agcacgctgt ggaattccat agttggtctc atccctggtc agtttccaca 120 tgatgatggt cttatctcga gaggcggaga ggatcatgtc cgggaactgc ggggtagtag 180 cgatctgggt tacccagccg ttgtggccct tgagggtgcc acgaagggtc atctgctcag 240 tcatggcggc ggcgagagcg tgtgtcgctg cagcgacgag gatggcactg gatggcttag 300 agaaactagc accacaacct ctcctgccgc acctgcccgg gcggcccgct cgaa 354 131 474 DNA Homo sapien misc_feature (1)...(474) n = A,T,C or G 131 cgagcggccg cccgggcagg tctggcagca gcttcctctg gaataattga cagctttgtg 60 ctgcctgact aaaatttgaa atgacaaccg ctgaatgtaa aatgatgtac ctacaatgag 120 agagatttag gaatactatc tgtcaatcca tagatgtaga aacaaaacaa actacagaat 180 gaaaacaaac ttattttaaa ccaaagaaac aaatgtatcc aaaatatagt ccatgatata 240 tttgattact agtataacca cagttgaaaa cttaaaaaaa aaaattgaca ttttttgtaa 300 tgggtactaa tggatttata aaaggtttct gtttccaaag atgttattgg ggtccacata 360 ttccttgaag acttcagcat cccaaagccc gacatcagag atactttcct ttagccattg 420 nttcccgtaa cttgcccact ccatggtgat gtgacaggct tcccttcatt agca 474 132 474 DNA Homo sapien misc_feature (1)...(474) n = A,T,C or G 132 ggccgaggtg gggaattcat gtggaggtca gagtggaagc aggtgtgaga gggtccagca 60 gaaggaaaca tggctgccaa agtgtttgag tccattggca agtttggcct ggccttagct 120 gttgcaggag gcgtggtgaa ctctgcctta tataatgtgg atgctgggca cagagctgtc 180 atctttgacc gattccgtgg agtgcaggac attgtggtag gggaagggac tcattttctc 240 atcccgtggg tacagaaacc aattatcttt gactgccgtt ctcgaccacg taatgtgcca 300 gtcatcactg gtagcaaaga tttacagaat gtcaacatca cactgcgcat cctcttccgg 360 cctgtcgcca gccagcttcc tcgcatcttc accagcatcg ganaggacta tgatgaaccg 420 tgtgctgccg tccatcacaa ctgagatcct caagtcagtg gtggctcgct ttga 474 133 387 DNA Homo sapien 133 tgctcgagcg gccgccagtg tgatggatat ctgcagaatt cggcttagcg tggtcgcggc 60 cgaggtctgc gggcccctta gcctgccctg cttccaagcg acggccatcc cagtagggga 120 ctttcccaca ctgtgccttt acgatcagcg tgacagagta gaagctggag tgcctcacca 180 cacggcccgg aaacagcggg aagtaactgg aaagagcttt aggacagctt agatgccgag 240 tgggcgaatg ccagaccaat gatacccaga gctacctgcc gccaacttgt tgagatgtgt 300 gtttgactgt gagagagtgt gtgtttgtgt gtgtgttttg ccatgaactg tggccccagt 360 gtatagtgtt tcagtggggg agaactg 387 134 401 DNA Homo sapien 134 ggccgcccgg gcaggtctga tgaagaacac gggtgtgatc cttgccaatg acgccaatgc 60 tgagcggctc aagagtgttg tgggcaactt gcatcggctg ggagtcacca acaccattat 120 cagccactat gatgggcgcc agttccccaa ggtggtgggg ggctttgacc gagtactgct 180 ggatgctccc tgcagtggca ctggggtcat ctccaaggat ccagccgtga agactaacaa 240 ggatgagaag gacatcctgc gcttgtgctc acctccagaa ggaagttgct cctgagtgct 300 attgactctt gtcaatgcga ccttcaagac aggaggctac ctggtttact gcacctgttc 360 tatcacagtg agacctctgc catggcagaa caggggaagc t 401 135 451 DNA Homo sapien 135 ggtcgcggcc gaggtctgtt cctgagaaca gcctgcattg gaatctacag agaggacaac 60 taatgtgagt gaggaagtga ctgtatgtgg actgtggaga aagtaagtca cgtgggccct 120 tgaggacctg gactgggtta ggaacagttg tactttcaga ggtgaggtgt cgagaaggga 180 aagtgaatgt ggtctggagt gtgtccttgg ccttggctcc acagggtgtg ctttcctctg 240 gggccgtcag ggagctcatc ccttgtgttc tgccagggtg gggtaccggg gtttgacact 300 gaggagggta acctgctggc tggagcggca gaacagtggc cttgatttgt cttttggaag 360 attttaaaaa ccaaaaagca taaacattct ggtccttcac aatgctttct ctgaagaaat 420 acttaacgga aggacttctc cattcaccat t 451 136 411 DNA Homo sapien 136 ggccgcccgg gcaggtctga atcacgtaga atttgaagat caagatgatg aagccagagt 60 tcagtatgag ggttttcgac ctgggatgta tgtccgcgtt gagattgaaa atgttccctg 120 tgaatttgtg cagaactttg acccccttta ccccattatc ctgggtggct tgggcaacag 180 tgagggaaat gttggacatg tgcaggtggg tccctttgct gcgtatttgg tgcctgaggc 240 tctgtggatt tcccctccat caatcatctt accctctcat ccccctcaga tgcgtctgaa 300 gaaacatctc tggtataaga aaatcctcaa gtcccaagat ccaatcatat tttctgtagg 360 gtggaggaag tttcagacca tcctgctcta ttatatccga agaccacaat g 411 137 211 DNA Homo sapien misc_feature (1)...(211) n = A,T,C or G 137 cggccgcccg ggcaggtcgg ttggtgcggc ctccattgtt cgtgttttaa ggcgccatga 60 ggggtgacag aggccgtggt cgtggtgggc gctttggttc cagaggaggc ccaggaggag 120 ggttcaggcc ctttgcacca catatcccat ttgacttcta tttgtgtgaa atggcctttc 180 cccggntcaa gccagcacct cgatgaaact t 211 138 471 DNA Homo sapien 138 gccgcccggg caggtctggg ctggcgactg gcatccaggc cgtaactgca aatctatgct 60 aggcggggtc tcccttctgt gtgttcaagt gttctcgact tggattctta actattttaa 120 aaaatgcact gagtttgggt taaaaaccaa ccaccaaaat ggatttcaac acagctctaa 180 agccaagggc gtggccggct ctcccaacac agcgactcct ggaggccagg tgcccatggg 240 cctacatccc ctctcagcac tgaacagtga gttgattttt ctttttacaa taaaaaaagc 300 tgagtaatat tgcataggag taccaagaaa ctgcctcatt ggaaacaaaa actatttaca 360 ttaaataaaa agcctggccg caggctgcgt ctgccacatt tacagcacgg tgcgatgcac 420 acggtgacca aaccacggag gcaagcttct ggcactcaca ccacgacccg c 471 139 481 DNA Homo sapien misc_feature (1)...(481) n = A,T,C or G 139 gtcgcggccg aggtctgttc tttagctcag atttaaacct gctgtctctt ctttatttgc 60 agaatgaatt cccagttcct gagcagttca agaccctatg gaacgggcag aagttggtca 120 ccacagtgac agaaattgct ggataagcga agtgccactg ggttctttgc cctcccttca 180 caccatggga taaatctgta tcaagacggt tcttttctag atttcctcta cctttttgct 240 cttaaaactg cttctctgct ctgagaagca cagctacctg ccttcactga aatatacctc 300 aggctgaaat ttggggtggg atagcaggtc agttgatctt ctgcaggaag gtgcagcttt 360 tccatatcag ctcaaccacg ccgncagtcc attcttaagg aactgccgac taggactgat 420 gatgcatttt agcttttgag cttttggggg gtattctacc aaccaacagt ccatttggaa 480 a 481 140 421 DNA Homo sapien misc_feature (1)...(421) n = A,T,C or G 140 gtcgcggccg aggtttccca tttaagaaaa atagatcttg agattctgat tcttttccaa 60 acagtcccct gctttcatgt acagcttttt ctttacctta cccaaaattc tggccttgaa 120 gcagttttcc tctatggctt tgcctttctg attttctcag aggctcgagt ctttaatata 180 accccaaatg aaagaaccaa ggggaggggt gggatggcac ttttttttgt tggtcttgtt 240 ttgttttgtt ttttggttgg ttgggttccg ttatttttta agattagcca ttctctgctg 300 ctatttccct acataatgtc aatttttaac cataattttg acatgattga gatgtacttg 360 aggctttttt gntttaattg agaaaagact ttgcaatttt ttttttagga tgagcctctc 420 c 421 141 242 DNA Homo sapien misc_feature (1)...(242) n = A,T,C or G 141 cgantngccc gcccgggcan gtctgtctaa ntttntcang gaccacgaac agaaactcgt 60 gcttcaccga anaacaatat cttaaacatc gaanaattta aatattatga aaaaaaacat 120 tgcaaaatat aaaataaata nnaaaaggaa aggaaacttt gaaccttatg taccgagcaa 180 atccaggtct agcaaacagt gctagtccta nattacttga tntacaacaa cacatgaata 240 ca 242 142 551 DNA Homo sapien misc_feature (1)...(551) n = A,T,C or G 142 agcgtggtcg cggcncgang tccacagggc anatattctt ttagtgtctg gaattaaaat 60 gtttgaggtt tangtttgcc attgtctttc caaaaggcca aataattcan atgtaaccac 120 accaagtgca aacctgtgct ttctatttca cgtactgttg tccatacagt tctaaataca 180 tgtgcagggg attgtagcta atgcattaca cagtcgttca gtcttctctg cagacacact 240 aagtgatcat accaacgtgt tatacactca actagaanat aataagcttt aatctgaggg 300 caagtacagt cctgacaaaa gggcaagttt gcataataga tcttcgatca attctctctc 360 caaggggccc gcaactaggc tattattcat aaaacacaac tgaanagggg attggtttta 420 ctggtaaatc atgtgntgct aaatcatttt ctgaacagtg gggtctaaat cantcattga 480 tttagtggca gccacctgcc cggcggccgn tcgaagccca attctgcaga tatccatcac 540 actggcggcc g 551 143 515 DNA Homo sapien misc_feature (1)...(515) n = A,T,C or G 143 cgagnggccc gcccgggcag gtatcttcac aaactcaaca aaggcactac atgagacttc 60 acattcccct agtccaatag ctgacaaatt tttgcaacgt tctgcaatgc gaattaactc 120 ttcatcaagt ggccgtaatc catttgcaca cactactagt tcaaccagtc tagggcatgt 180 cattcccaca cggccaagca catctttgct tactgatctc ccaaagtaca gatgggtggc 240 aggtatttca tagcgaaaga aggggtcaaa ttcttcttca tataanaaaa aatacatcac 300 taagttcact ttgggtgaat gtctgatgaa agcatcccag ctactcttct gaatagtatg 360 gaagtgtgtc tgtccaggat tctcactgac tacatcaatg cgcaaatgtt ctaatcgaac 420 atgtttttca gaagacaatg caagtaacaa ctcatcactc aataagtggt aagttcaggg 480 ctagttctct taagccgnga cactgatcag cacac 515 144 247 DNA Homo sapien misc_feature (1)...(247) n = A,T,C or G 144 tgcattctct ntggatgcan acctgcccgt tggtagggac tntgctcaca cggaacatgg 60 acggttacac ctgtgccgtg ggtgacgtcc accagcttct ggatcatctc ggcgngggtg 120 ttgtggaagg gcagactatc cacctccatg cncacgatgc ccganacgcc actccggact 180 ntgtgctgca ccaanatgcc cagcattnta tcttcaagca nagcacttat cagggtcctt 240 ggcacac 247 145 309 DNA Homo sapien misc_feature (1)...(309) n = A,T,C or G 145 cgtgggtcgc ggcccgangt ctgctgtaac aaaacaccat agtctgggca gctcatagac 60 aatggaattt tatttctcac gcttctggag gctggattcc aagatcaagg ttccaggaga 120 ctcagtgtct ggcaaggtct cggtttctgc ctcanagatg gtgccatctg gctgtgtcct 180 cacaagtagg aaggtgcaag aagctcccct caggctctgt ctgtaagaca ctgatcccat 240 tcatganggg gaaacgtaat gacctaatca gcccccagag accccacttc taacaccatc 300 accttgggg 309 146 486 DNA Homo sapien misc_feature (1)...(486) n = A,T,C or G 146 agcgtgggtc gcggcncgac gtcctgtcca tatttcacag cccgagaact aatacaagat 60 gctgacatca tattttgtcc ctacaactat cttctanatg cacaaataag ggaaagtatg 120 gatttaaatc tgaaagaaca ggttgtcatt ttanatgaag ctcataacat cgaggactgt 180 gctcgggaat cagcaagtta cagtgtaaca gaagttcagc ttcggtttgc tcgggatgaa 240 ctanatagta tggtcaacaa taatataagg aaganagatc atgaacccct acgagctgtg 300 tgctgtagcc tcattaattg gntagaagca aacgctgaat atcttgnana angagantat 360 gaatcagctt gtaaaatatg gagtggaaat gaaatgctct taactttaca caaaatgggt 420 atcaccactg ctacttttcc cattttgcng gtaagatatn ttttctacct gngaaacgta 480 tttaag 486 147 430 DNA Homo sapien misc_feature (1)...(430) n = A,T,C or G 147 gccgcccggg cangttcgac attacntnga gttccatgat gtacaattct ttcacgaaaa 60 acaatgaatg caagaatttg aggatctcct tactcctccc ttttacagat ggtctctcaa 120 tcccttcttc ttcctcttca tcttcatctt cttctgaacg cgctgccggg taccacggct 180 ttctttgtct ttatcgtgag atgaaggtga tgcttctgtt tcttctacca taactgaaga 240 aatttcgctg caagtctctt gactggctgt ttctccgact tcgcctttnt gtcaaacgng 300 agtcttttta cctcatgccc ctcagcttca cagcatcttc atctggatgt tnatttctca 360 aagggctcac tgaggaaact tctgattcan atgtcgaana gcactgtgaa gttttctctt 420 cattttgctg 430 148 483 DNA Homo sapien misc_feature (1)...(483) n = A,T,C or G 148 cccgggcagg tctgtgttgn tttncaaccg gtgtcctccc cagcgtccag aananggaaa 60 tgtggagcgg gtgatgatga cccctcgctg tcctgtcacc tcctgcacag cttcgtatgt 120 gggtctggtc tgggaccacc cgtacaggtt gtgcacgttg tagtgctcca cgggggagct 180 gtccggcagg atctgctgac tctccatgca cagagtcttg ctgctcaggc ccttgtccct 240 agattccaaa tatggcatat agggtggggt tatttagcat ttcattgctg cagcccctga 300 cagatccatc cacaaaattt gatggctcat tcatatcaat ccacaatcca tcaaacttca 360 agctcttctc tggntctcga nggtttgcat agaactcttc tatctctttc ttccaccacg 420 canacctcgg ncgcgaccac gctaagccga attctgcana tatccatcac actggcggcc 480 gct 483 149 439 DNA Homo sapien misc_feature (1)...(439) n = A,T,C or G 149 ctttcacgaa nacaatgaat gcaagaattt gaggatctcc ttactcctcc cttttacaga 60 tggtctctca atcccttctt cttcctcttc atcttcatct tcttctgaac gcgctgccgg 120 gtaccacggc tttctttgtc tttatcgtga gatgaaggtg atgcttctgt ttcttctacc 180 ataactgaag aaatttcgct gcaagtctct tgactggctg tttctccgac ttcgcctttt 240 tgcaaacgtg agtcttttta cctcatgccc ctcagcttcc acagcatctt catctggatg 300 ttcatttctc aaagggctca ctgaggaaac ttctgactca catgtcgaag aagcactgng 360 agtttctctt catttgctgc aaanttgctc tttgctggct gngctctcag accacccatt 420 tggctgcatg ggggctgac 439 150 578 DNA Homo sapien misc_feature (1)...(578) n = A,T,C or G 150 ggcncgcccg ggcangtcca ctccactttt gagctctgag ggaatacctt caggagggac 60 agggtcaggg agtcctggca gctccgcagc agagattcac attcattcag agacttgttg 120 tccagtgcaa tgccattgat cgcaacgatc ctgtctccca cagcaaggga cccttcttta 180 gcggcagggc ttccaggcag cacagcggca gcatacactc cattctccag actgatgcca 240 ctgtctttct gtccactgan gttgatgtgc agcggcgtga ccaccttccc acccagggac 300 ttcctccgcc gcacgaccat gttgatgggc cccctnccca ttgaggagcg ccttgatggc 360 ctgcttcttg nccttggtga tgaagtccac atcggtgatt ctcacagcca gtcattgacc 420 cttaagcggn catcagcaat gcttcctttg gccactttag ngacaaatat gccacagtcc 480 ccgggaaaca agggtcattc acaccttctg gcatatcaaa cacctcggcc gggancacta 540 agccgaattc tgcagatatc catcacactg gngggccg 578 151 503 DNA Homo sapien misc_feature (1)...(503) n = A,T,C or G 151 cgagcggccc gcccgggcag gtctgggaga tcagcgactg ctgccacgtg cccagaaatg 60 gctcgtcctt tcactacagc ggaatgcaat gagggtgggt gagaagatga tgggtcggtt 120 atttcattcc ttttcttttt acaacttcac tttcagagac ttcagcgttc catgtctgct 180 gtgctgtgga acccagagtg ctcttgcctg gatggctgag aatcccttgg accctggaag 240 cacctactcc atgatggccc ggtatagtgc aggctcaata taatcttccc ggtatcttga 300 gttgataact cgttgccgtt tcttttcttg cttaacctct ttctctgtga aaatctcatt 360 gaagcgcatg tctgaagcta ctgacagtct anatttgact ctcttgggaa gctcttcatc 420 cagtgtgtat acatcatctc tcttaaccac aagttggagc catncttaaa cttcacctgg 480 tacatttgga tagggtggga ggc 503 152 553 DNA Homo sapien misc_feature (1)...(553) n = A,T,C or G 152 agcgtggtcg cggcccgagg tccactgagc tccgccttcc ccgggctccc tgaggaagca 60 gagtcctgac ttccaggaag gacaggacac agaggcaaga actcagcctg tgaggctctg 120 ggtggctcct gaggccagag gacgccttcc gcgatccatg gctcagcatc gtccttctgg 180 cttcccagcc ccgggccgaa cgttcgggtt aataagcaga gcagttattc ggctcctggc 240 aggagctccc ccgttagttt ccacgttgtg agcacattca tacttaagac tgnttctctt 300 tgtgttttaa gcgtctgtct ctgtagtaaa ctgaaatgtt aacagaaatg cagacctgcc 360 cgggcggccg ctcgaaagcc gaattctgca gatatccatc acactggcgg ccgctcgagc 420 atgcatctag anggcccaat tcgccctata gtgagtcgna ttacaattca ctgggccgcg 480 ntttacaacg tcgtgactgg gaaaaccctg cggtacccac ttaatcgcct tgcagnacat 540 ccccctttcg cca 553 153 454 DNA Homo sapien misc_feature (1)...(454) n = A,T,C or G 153 tcgagcggct cgcccgggca ggtccaccta gcatggctcc tctaaacacg caactcagcg 60 aggggacccc cttcacctct ggcaagagag ctgggtagat cagaaacttg gtgacacctg 120 gctagcacag agcaggctca cttgtcttgg tcccactacc cagattcctg cagacattgc 180 aaaccaaatg aaggttgntg aatgacccct gtccccagcc acttgttttg gtatcatctg 240 ctctgcagtg gaatgcctgt gtgtttgagt tcactctgca tctgtatatt tgagtataga 300 aaccgantca agtgatctgt gcatncagac acactggggc acctgancac agaacaaatc 360 accttaacga tctggaatga aactgnganc antgcccgcc tgggtgggtc tgganaaact 420 gccgncttct tgttggacct tggccgcacc acct 454 154 596 DNA Homo sapien misc_feature (1)...(596) n = A,T,C or G 154 agcgtggtcg cggcccgang gcggcctcct gantganggg aagggacgtg ggggcggcca 60 cggcaggatt aacctccatt tcagctaatc atgggagaga ttaaagtctc tcctgattat 120 aactggttta naggtacagt tccccttaaa aagattattg tggatgatga tgacagtaag 180 atatggtcgc tctatgacgc gggcccccga agtatcaggt gtcctctcat attcctgccc 240 cctgtcagtg gaactgcaga tgtctttttc cggcagattt tggctctgac tggatggggt 300 taccgggtta tcgctttgca gtatccagtt tattgggacc atctcgagtt cttgtgatgg 360 attcacaaaa cttttanacc atttacaatt ggataaagtt catctttttg gcgcttcttt 420 gggangcttt ttggcccana aatttgctga atacactcac aaatctccta gaagccattc 480 cctaatcctc tgcaattcct tcagngacac ctctatcttc aaccaacttg gactggaaac 540 agctttggct gatgcctgca tttatgctca aaaaatagtt cttggaaatt ttcatc 596 155 343 DNA Homo sapien misc_feature (1)...(343) n = A,T,C or G 155 ctcganttgg cncgcccggg cangtctgcc tggtttttga ccgngcgagc tatttagnct 60 ctggctctgt ttccggagct caaggnaaaa atcttgaana actcgagcag cttctgtgga 120 tagccttggg tacacatact gccgagcata gccaatgtac tttctcaata gctggtgggg 180 aatgggatct attgtttctc caggaaccac ctttagtctt tctgataatg gcttctcaga 240 aactacttca agtacggaag tatttgaatc ttgactatnc atacgagcta ctgtggcact 300 gctaatgggn tctctgctnt ccagctctta ttgcaatcac atg 343 156 556 DNA Homo sapien misc_feature (1)...(556) n = A,T,C or G 156 tcgagcggcc cgcccgggca ggtctggcac cacncagatc gattaactgg ctcatctgat 60 ctcgtggccc ccaccctgga actgacttag cacaaaagga cacctcaatt ccttatgatt 120 tcatctccga cccaaccaat caacaccctt gactcactgg ccttccccct cccaccaaat 180 tatccttaaa aactctgatc cccgaatgct cagggagatc gatttgagta ctaataagac 240 tccagtctcc tgcacaagca gctctgtgta ctcttcctct attgcaattc ctgtcttgat 300 aaatcggctc tgtgtaggcg gcggaagaag tgaacctgtt gggcggttac cacctctgtc 360 gtgtgtgaca gttgntttga atctctaatt gctcagtaca gatccacatg caggttaagt 420 aagaagcttt tgaagaaaat ggaaagtctt aagtgatggc ttccaagaaa tcaaacctac 480 attaattagg gaacaacgga ctttacgtat cacaaatgaa gagactgacn aagtaaatca 540 acttggcctt ttctta 556 157 333 DNA Homo sapien misc_feature (1)...(333) n = A,T,C or G 157 ggtccacaaa aatatatnaa ataagctgga tatataaaan caaacactta acatngncan 60 cattccttca gttattcaaa ctcactgata nctaacnggg agnagttggn attctggaag 120 acttcctaag ctaaaagtat atttacatat ttacaacaca ngtaaatata acngaagaac 180 tacttcaaat aangnngaaa ttccagaatt ctanagattt atagctatag ntnacaanta 240 tcaccaattg gtttgcaatc aanngnccag cactacttat gannaangtt taactannaa 300 accaaaaggg gagaaaacct ggnagggaaa nat 333 158 629 DNA Homo sapien misc_feature (1)...(629) n = A,T,C or G 158 tcgagcggcc gcccgggcag gtctggtaca tttgtgcgag gtccggcact ctgttctcat 60 ccagtaagtg gtcgagccct ttctgcagaa ttgctgttaa atgttctcct aatagctgtt 120 tctccacaca agcaatcagt ggtttctgtg tgctgtggtc caagtaagtg attactctgt 180 ctccctcttc ttctaagcgt ttacttacat ggttaagata ttctggaacc tctctttcct 240 gcattaacct ttggccttcg gcagcatata agcaattagt ctcttccaaa aatttcagtt 300 caaatgaatc tttatacacc tgcaggtcag acagcatgcc caggnaggct ccgcaacagg 360 ctccggtcca cggcctcgcc gctcctctcg cgctcgatca gcagtaggat tccatcaatg 420 gttttactct gaaccatttt atcactaata atatgggttc taaacagttc taatcccata 480 tcccagatgg agggcagcgt ggagttctgc agcacatagg tgcggtccaa gaacaggaag 540 atgcttctga tcatgaatca tttgnctggc aatggtcctg ccagcacgtg gtaatctttc 600 ttttaaaaat aaacccttat ctaaacgtc 629 159 629 DNA Homo sapien misc_feature (1)...(629) n = A,T,C or G 159 tcgagcggcc gcccgggcag gttctagagg ganaatctgg ctgatttggg aataaaatat 60 aatcgaatat tcaacaccat gaagataaat cttattttgg aaatctactg accttaatac 120 cccaagcttg ccctgaatac tttgattgga attggaatat atcaaaaaag gttagtattt 180 ttgttgtagt taggatacta aaaggatatt agttacccaa gagatccaat ttgtttttct 240 gatgaatagt gttcagtaaa atgaagcagt cttaagagtg actaataatt tcaaagtgat 300 ttttcgtcta ttcttaatat tttttaatta tttattttta agagttttat accttgagca 360 gatacaatga tccgctttag tgagaggaca atttctgatt gattgttttc tcttcaggcc 420 atctcacctc ttcattctct tgttacattt gaagcagttg atataatggg tttatacttt 480 aaaagataga catggtgcca tgaagtttgg ggaagttggg tgaattatcc cattctagtt 540 acagangagc tttccttaaa tgccctttac ttctangttt ggtcaagaag tcattttctg 600 agtaaaagtt attttcatat atgttgggg 629 160 519 DNA Homo sapien misc_feature (1)...(519) n = A,T,C or G 160 tcgagcggcg cgcccgggca ggtctgctgg gattaatgcc aagttnttca gccataaggt 60 agcgaaatct agcagaatcc agattacatc cacttccaat cacgcggtgt ttgggtaatc 120 cacttagttt ccagataaca tacgtaagaa tgtccactgg gttggaaacc acaattatga 180 tgcaatcagg actgtacttg acgatctgag gaataatgaa tttgaagaca ttaacatttc 240 tctgcaccag attgagccga ctctcccctt cttgctgacg gactcctgca gttaccacta 300 caatcttana attgggcggg tcacagaata atctttatct gccacaattt taggtgctga 360 agaaataagc tcccatgctg cagatccatc atttctnctt taagcttatc ttccaaaaca 420 tccacaagan caangttcat cagccagaga ctttcccaga atgctgatag nacacgccat 480 accaacttgt ccaacancca ctacagcgat cttattggt 519 161 446 DNA Homo sapien misc_feature (1)...(446) n = A,T,C or G 161 cgagnggccc gcccgggcag gtccagtaag cntttnacga tgatgggaaa ggttatgcaa 60 ggtcccagcg gtacaacgag ctgtttctac atcatttgta ttctgcatgg tacgtacaat 120 agcagacacc atctgaggag aacgcatgat agcgtgtctg gaagcttcct ttttagaaag 180 ctgatggacc ataactgcag ccttattaac caccacctgg tcctcgtcat ttagcagttt 240 tgtcagttca gggattgcac gtgtggcang ttctgcatca tcttgatagt taatcaagtt 300 tacaactggc atgtttcagc atctgcgatg ggctcagcaa acgctggaca ttantgggat 360 gagcagcatc aaactgtgta natgggatct gcatgccctc atctaatgtc tcagggaaca 420 tagcagctcg taccctctga gctcga 446 162 354 DNA Homo sapien misc_feature (1)...(354) n = A,T,C or G 162 agcgtngtcg cggcccgang tcctgggaag cctttnttgc tgagcctcac agcctctgtc 60 aggcggctgc ggatccagcg gtccaccagg ctctcatggc ctccgggctg ggaggngggt 120 gagggcacaa aacccttccc aaggccacga anggcaaact tggtggcatt ccanagcttg 180 ttgcanaagt ggcggnaacc cagtatccgg ttcacatcca ggntgatgtc acgaccctgg 240 gacatgtang cacataatcc aaaccggaga gcatcggtgc cacattcacg aatccccgct 300 gggaagtcag ctttctgccc ttctttggcc ttctccacct cgctgggatc cagg 354 163 258 DNA Homo sapien misc_feature (1)...(258) n = A,T,C or G 163 tttttcncca agtcctcttg ccgngggatc tngactgcaa tttaagacac ttctaattag 60 ttatacccag gccctgcaaa attgctgggt ttatataata tattcttgct gcacgaagat 120 ttattattct gttggatgat tctattttaa ttntatttat tctggccaaa aaagaacctt 180 ctccgctcgt caagagangc caatntgtct tgaaggacaa gagaaagatg ctaacacaca 240 ctttcttctt cttgagga 258 164 282 DNA Homo sapien misc_feature (1)...(282) n = A,T,C or G 164 ggaacatatt acttttaaat tacttgggtc aatgaaacat ttaataaaaa catttgcttc 60 tctatataat acgtatgtat aaaataagcc ttttcanaaa ctctggttct cataatcctc 120 tataaatcan atgatctgac ttctaagagg aacaaattac agnaaggggt atacattnat 180 gaatactggt agtactagag ganngacgct aaaccactct actaccactt gcggaactct 240 cacagggtaa atgacaaagc caatgactga ctctaaaaac aa 282 165 462 DNA Homo sapien misc_feature (1)...(462) n = A,T,C or G 165 gcccgggcan gtcctgtaat cccagctact cangangctg agtcatgana atcgcctgaa 60 tccgggaggt agaggccgca gcgagcaaag attaagccac tgcactccag tctgggtgac 120 agagtgagaa tctgtctgtt gctcctctgg cattggtctg aaatgggttt gtagaacatg 180 ccacagaagg accagcanca gcaacaaatg gatttgtgga angcgtagct ccaaatggag 240 cangcacact tgatgaagca cgctgtgtct gtgcagangc aaccactggc actgttccaa 300 aaacattgct gctagcatta cttgtggaag tatacgcatt actggaggtg gctgcanaac 360 tgaaaacgct gtctagttct gccanagctg catacttgnc tgaanatgca cttgactgac 420 tgggaactga accacanaac caacaggacc tttacctgtg ga 462 166 365 DNA Homo sapien misc_feature (1)...(365) n = A,T,C or G 166 cgtgggtcgc ggcncgangt ctgaaaccaa tccagaacta aacatcagca cacaaaaaat 60 accaggatag atggaatcaa aagactctga agccaaaagg aggctaggga gagcaactga 120 acttagcaag ctgaggactt cagtgtccat catccgatcc tgccctgtaa caacaggtct 180 atatgataga gatattccat ctgagctgga ggccattatc cttagcaaac taacacagaa 240 cagaaaacca aatacatgtt ctcatttaga agtaggagct aaatgatgag aactcaagga 300 cacaaagaaa ggaacaacag acactggggc ctacttgagg gtggagggtg ggaggaggga 360 gaaga 365 167 364 DNA Homo sapien misc_feature (1)...(364) n = A,T,C or G 167 agcgtggtcg cggcgcgang tccagcccta gcttgcctgt gactccgcct tcactgggtg 60 ctctctctaa aagttgctga ctctttactg tatctcccaa ttcccactcc attggttcca 120 taaggggagg ggtgtctcac tcaacatggt gttcctggta ccaagaactg gctgacgaag 180 ctgggtgccg tggctcatgc ctgtaatccc agcacttttg ggaggccaag aagggcggat 240 cacctgaggt ctggagttca agatcagcct gaccaacatg atgaaaccaa gtctccacta 300 aaaatataaa acaattagcc aggcatggtg gtgggtgcct gnaatcccag ctactgggga 360 ngct 364 168 447 DNA Homo sapien misc_feature (1)...(447) n = A,T,C or G 168 cccgggcagg tcaaaaccca aaacctttca ttttagccca aaccagctca tgattaggta 60 tacaaggata acagaaccag ttgtcaggac gagcatttga caagtaaaag caattcttgc 120 aaagctgcag ttcatccagc tcatggcatg tgtctttata tagcatcctc gcaatgtcag 180 cttgctcact gtctgctcca tagaaaatca cggtattgtg gagaagcaat tgggcatcag 240 ctttgaactc ttcataactt cggtatttcc cttcattcac tttctcttga atggtgggaa 300 cgtccacaga cctcggccgc gaccacgcta agcccgaatt ctgcagatat ccatcacact 360 ggcggccgtt cgagcatggc atctagaagg cccaattcgc ctatagngag tcgnattacc 420 aattcactgg ccgtcgnttt acaacgc 447 169 524 DNA Homo sapien misc_feature (1)...(524) n = A,T,C or G 169 cgantngcgc gcccgggcag gtctgagcag cctttctgnn tgctggacta ttgggattgg 60 gttcatccaa cagagactgt atggatgtta gaatggaaga cacatcatag gttggactcc 120 aacggttctg aagtatgtcc agacatatac taccatctgc atagactaag aacaaagaag 180 taggtacatt aaacgtaaca agaccactaa ggttttaaca ttatagacaa aacanaaata 240 gtcaaganta ctttgctttt gaagtttaaa gattcctatg ttgcttccca gttaactgcc 300 taaaaagata agncataacc accactagtg aaataatcan gatgatcaga gaatgtcana 360 tgtgatcagt ataaaactgg angatattna gtgtcatcct ttggaaaagg ctgccctatn 420 atccaggaaa tcanaaacat tnttgaacag ggnccctagc tatccacaga catgtgggaa 480 attcattccc caaatngtag gctggatccc ctatctgaaa taac 524 170 332 DNA Homo sapien misc_feature (1)...(332) n = A,T,C or G 170 tcgancggcn cgcccgggca ggtgacaaac ctgttattga agatgttggt tctgatgagg 60 aanaanatca gaagggatgg tgacaagaan aanaanaaga agattaagga aaagtacatc 120 gatcaagaag agctcaacaa aacaaagccc atctggacca gaaatcccga cgatattact 180 aatgangagt acggagaatt ctataanagc ttgaccaatg actgggaaga tcacttggca 240 gtgaagcatt tttcagttga nggacagttg gaattcagag cccttctatn tgtcccacga 300 cgtgctcctt ttgatctgtt tganancaga aa 332 171 334 DNA Homo sapien misc_feature (1)...(334) n = A,T,C or G 171 cgagnggcnc gcccgggcag gtctgttgat agcgacttaa cagaaaagtc tagacaaaca 60 taagcataaa aaattacagt ctttctaccc ttgggaatgg ggagaaaaag gaatctctac 120 cccaagacca gaaataataa gtcctgtttc tggtcctgaa catccagaat tatggaggct 180 ttggcctgac accacattan aatttggtct ggaaatcaaa ctttaganac angagatcgt 240 aagccatttt atactatcga cctaaattcc agtctaacgg ttcctttaca aagttgcgga 300 aagccctctt atatgctagc tgtaggaaat atag 334 172 439 DNA Homo sapien misc_feature (1)...(439) n = A,T,C or G 172 agcgtggtcg cggcccgang tctgcctata aaactagact tctgacgctg ggctccagct 60 tcattctcac aggtcatcat cctcatccgg gagagcagtt gtctgagcaa cctctaagtc 120 gtgctcatac tgtgctgcca aagctgggtc catgacaact tctggtgggg cgagagcagg 180 catggcaaca aattccaagt tagggtctcc aatgagcttc ctagcaagcc agaggaaggg 240 cttttcaaag ttgtagttac ttttggcaga aatgtcgtag tactgaagat tcttctttcg 300 gtggaagaca atggatttcg ccttcacttt ctgccttaat atccactttg gtgccacaca 360 acacaatggg gatgntttca cacacttngn accanatctc tatgccagnt aggccatttt 420 ggaagnactt cganggtac 439 173 599 DNA Homo sapien misc_feature (1)...(599) n = A,T,C or G 173 cgatnggccg cccgggcagg tcctgtaaaa naggaaattc agacatcgta cgactcgtaa 60 ttgaatgtgg agctgactgc aatattttgt caaagcacca gaatagtgcc ctgcactttg 120 cgaagcagtc taacaatgtg cttgtgtacg acttgctgaa gaaccattta gagacacttt 180 caagagtagc agaagagaca ataaaggatt actttgaagc tcgccttgct ctgctagaac 240 cagtttttcc aatcgcatgt catcgactct gtgagggtcc agatttttca acagatttca 300 attaccaacc cccacagaac ataccagaag gctctggcat cctgctgttt atcttccatg 360 caaacttttt gggtaaagaa gttattgctc ggctctgtgg accgtgtagt gtacaagctg 420 tagttctgaa tgataaattt cagcttcctg tttttctggg tctcgctctg ttgtccaggc 480 tggagtgcag tggcgcggat tacagctcac tggagtcttg acttcccagg cacaagcaat 540 cctcccacct cagcctccta actacctggg actaaaaatg caccgccacc acattccgg 599 174 458 DNA Homo sapien misc_feature (1)...(458) n = A,T,C or G 174 tcgatttggc cgcccgggca ggtccatgcn gnttntgccc attcccatgg ngcccgacaa 60 ncccatcccc gaggccgaca tccccatgtt catgttcatg cccaccatgc cctggctcat 120 ccctgcgctg ttccccagag gggccattcc catggtgccc gtcattacac cgggcatgtt 180 cataggcatg ggtcccccca ggagagggtt agnttgaggc cggacaggaa gcatgtttga 240 tggagaactg aggttcacag nctccaaaac tttgagtcat cacattcata ggctgctgca 300 tattctgtct gctgaatcca ttgtatncag tgatggcctg ctggggnttt ggaaggctng 360 cataccaggt agtaagntcg tctaggctga tgtttacacc tggggtcaga ccaagtanga 420 gggcaaggtt ttgctgactg attttctgga cccatatc 458 175 1206 DNA Homo sapien 175 ggcacgagga agttttgtgt actgaaaaag aaactgtcag aagcaaaaga aataaaatca 60 cagttagaga accaaaaagt taaatgggaa caagagctct gcagtgtgag gtttctcaca 120 ctcatgaaaa tgaaaattat ctcttacatg aaaattgcat gttgaaaaag gaaattgcca 180 tgctaaaact ggaaatagcc acactgaaac accaatacca ggaaaaggaa aataaatact 240 ttgaggacat taagatttta aaagaaaaga atgctgaact tcagatgacc ctaaaactga 300 aagaggaatc attaactaaa agggcatctc aatatagtgg gcagcttaaa gttctgatag 360 ctgagaacac aatgctcact tctaaattga aggaaaaaca agacaaagaa atactagagg 420 cagaaattga atcacaccat cctagactgg cttctgctgt acaagaccat gatcaaattg 480 tgacatcaag aaaaagtcaa gaacctgctt tccacattgc aggagatgct tgtttgcaaa 540 gaaaaatgaa tgttgatgtg agtagtacga tatataacaa tgaggtgctc catcaaccac 600 tttctgaagc tcaaaggaaa tccaaaagcc taaaaattaa tctcaattat gccggagatg 660 ctctaagaga aaatacattg gtttcagaac atgcacaaag agaccaacgt gaaacacagt 720 gtcaaatgaa ggaagctgaa cacatgtatc aaaacgaaca agataatgtg aacaaacaca 780 ctgaacagca ggagtctcta gatcagaaat tatttcaact acaaagcaaa aatatgtggc 840 ttcaacagca attagttcat gcacataaga aagctgacaa caaaagcaag ataacaattg 900 atattcattt tcttgagagg aaaatgcaac atcatctcct aaaagagaaa aatgaggaga 960 tatttaatta caataaccat ttaaaaaacc gtatatatca atatgaaaaa gagaaagcag 1020 aaacagaagt tatataatag tataacactg ccaaggagcg gattatctca tcttcatcct 1080 gtaattccag tgtttgtcac gtggttgttg aataaatgaa taaagaatga gaaaaccaga 1140 agctctgata cataatcata atgataatta tttcaatgca caactacggg tggtgctgct 1200 cgtgcc 1206 176 317 PRT Homo sapien 176 Met Gly Thr Arg Ala Leu Gln Cys Glu Val Ser His Thr His Glu Asn 1 5 10 15 Glu Asn Tyr Leu Leu His Glu Asn Cys Met Leu Lys Lys Glu Ile Ala 20 25 30 Met Leu Lys Leu Glu Ile Ala Thr Leu Lys His Gln Tyr Gln Glu Lys 35 40 45 Glu Asn Lys Tyr Phe Glu Asp Ile Lys Ile Leu Lys Glu Lys Asn Ala 50 55 60 Glu Leu Gln Met Thr Leu Lys Leu Lys Glu Glu Ser Leu Thr Lys Arg 65 70 75 80 Ala Ser Gln Tyr Ser Gly Gln Leu Lys Val Leu Ile Ala Glu Asn Thr 85 90 95 Met Leu Thr Ser Lys Leu Lys Glu Lys Gln Asp Lys Glu Ile Leu Glu 100 105 110 Ala Glu Ile Glu Ser His His Pro Arg Leu Ala Ser Ala Val Gln Asp 115 120 125 His Asp Gln Ile Val Thr Ser Arg Lys Ser Gln Glu Pro Ala Phe His 130 135 140 Ile Ala Gly Asp Ala Cys Leu Gln Arg Lys Met Asn Val Asp Val Ser 145 150 155 160 Ser Thr Ile Tyr Asn Asn Glu Val Leu His Gln Pro Leu Ser Glu Ala 165 170 175 Gln Arg Lys Ser Lys Ser Leu Lys Ile Asn Leu Asn Tyr Ala Gly Asp 180 185 190 Ala Leu Arg Glu Asn Thr Leu Val Ser Glu His Ala Gln Arg Asp Gln 195 200 205 Arg Glu Thr Gln Cys Gln Met Lys Glu Ala Glu His Met Tyr Gln Asn 210 215 220 Glu Gln Asp Asn Val Asn Lys His Thr Glu Gln Gln Glu Ser Leu Asp 225 230 235 240 Gln Lys Leu Phe Gln Leu Gln Ser Lys Asn Met Trp Leu Gln Gln Gln 245 250 255 Leu Val His Ala His Lys Lys Ala Asp Asn Lys Ser Lys Ile Thr Ile 260 265 270 Asp Ile His Phe Leu Glu Arg Lys Met Gln His His Leu Leu Lys Glu 275 280 285 Lys Asn Glu Glu Ile Phe Asn Tyr Asn Asn His Leu Lys Asn Arg Ile 290 295 300 Tyr Gln Tyr Glu Lys Glu Lys Ala Glu Thr Glu Val Ile 305 310 315 177 20 DNA Artificial Sequence Made in the Lab 177 ccaatcatct ccacaggagc 20 178 1665 DNA Homo sapien 178 gcaaactttc aagcagagcc tcccgagaag ccatctgcct tcgagcctgc cattgaaatg 60 caaaagtctg ttccaaataa agccttggaa ttgaagaatg aacaaacatt gagagcagat 120 cagatgttcc cttcagaatc aaaacaaaag aaggttgaag aaaattcttg ggattctgag 180 agtctccgtg agactgtttc acagaaggat gtgtgtgtac ccaaggctac acatcaaaaa 240 gaaatggata aaataagtgg aaaattagaa gattcaacta gcctatcaaa aatcttggat 300 acagttcatt cttgtgaaag agcaagggaa cttcaaaaag atcactgtga acaacgtaca 360 ggaaaaatgg aacaaatgaa aaagaagttt tgtgtactga aaaagaaact gtcagaagca 420 aaagaaataa aatcacagtt agagaaccaa aaagttaaat gggaacaaga gctctgcagt 480 gtgaggtttc tcacactcat gaaaatgaaa attatctctt acatgaaaat tgcatgttga 540 aaaaggaaat tgccatgcta aaactggaaa tagccacact gaaacaccaa taccaggaaa 600 aggaaaataa atactttgag gacattaaga ttttaaaaga aaagaatgct gaacttcaga 660 tgaccctaaa actgaaagag gaatcattaa ctaaaagggc atctcaatat agtgggcagc 720 ttaaagttct gatagctgag aacacaatgc tcacttctaa attgaaggaa aaacaagaca 780 aagaaatact agaggcagaa attgaatcac accatcctag actggcttct gctgtacaag 840 accatgatca aattgtgaca tcaagaaaaa gtcaagaacc tgctttccac attgcaggag 900 atgcttgttt gcaaagaaaa atgaatgttg atgtgagtag tacgatatat aacaatgagg 960 tgctccatca accactttct gaagctcaaa ggaaatccaa aagcctaaaa attaatctca 1020 attatgccgg agatgctcta agagaaaata cattggtttc agaacatgca caaagagacc 1080 aacgtgaaac acagtgtcaa atgaaggaag ctgaacacat gtatcaaaac gaacaagata 1140 atgtgaacaa acacactgaa cagcaggagt ctctagatca gaaattattt caactacaaa 1200 gcaaaaatat gtggcttcaa cagcaattag ttcatgcaca taagaaagct gacaacaaaa 1260 gcaagataac aattgatatt cattttcttg agaggaaaat gcaacatcat ctcctaaaag 1320 agaaaaatga ggagatattt aattacaata accatttaaa aaaccgtata tatcaatatg 1380 aaaaagagaa agcagaaaca gaaaactcat gagagacaag cagtaagaaa cttcttttgg 1440 agaaacaaca gaccagatct ttactcacaa ctcatgctag gaggccagtc ctagcattac 1500 cttatgttga aaatcttacc aatagtctgt gtcaacagaa tacttatttt agaagaaaaa 1560 ttcatgattt cttcctgaag cctgggcgac agagcgagac tctgtctcaa aaaaaaaaaa 1620 aaaaaaagaa agaaagaaat gcctgtgctt acttcgcttc ccagg 1665 179 179 PRT Homo sapien 179 Ala Asn Phe Gln Ala Glu Pro Pro Glu Lys Pro Ser Ala Phe Glu Pro 1 5 10 15 Ala Ile Glu Met Gln Lys Ser Val Pro Asn Lys Ala Leu Glu Leu Lys 20 25 30 Asn Glu Gln Thr Leu Arg Ala Asp Gln Met Phe Pro Ser Glu Ser Lys 35 40 45 Gln Lys Lys Val Glu Glu Asn Ser Trp Asp Ser Glu Ser Leu Arg Glu 50 55 60 Thr Val Ser Gln Lys Asp Val Cys Val Pro Lys Ala Thr His Gln Lys 65 70 75 80 Glu Met Asp Lys Ile Ser Gly Lys Leu Glu Asp Ser Thr Ser Leu Ser 85 90 95 Lys Ile Leu Asp Thr Val His Ser Cys Glu Arg Ala Arg Glu Leu Gln 100 105 110 Lys Asp His Cys Glu Gln Arg Thr Gly Lys Met Glu Gln Met Lys Lys 115 120 125 Lys Phe Cys Val Leu Lys Lys Lys Leu Ser Glu Ala Lys Glu Ile Lys 130 135 140 Ser Gln Leu Glu Asn Gln Lys Val Lys Trp Glu Gln Glu Leu Cys Ser 145 150 155 160 Val Arg Phe Leu Thr Leu Met Lys Met Lys Ile Ile Ser Tyr Met Lys 165 170 175 Ile Ala Cys 180 1681 DNA Homo sapien 180 gatacagtca ttcttgtgaa agagcaaggg aacttcaaaa agatcactgt gaacaacgta 60 caggaaaaat ggaacaaatg aaaaagaagt tttgtgtact gaaaaagaaa ctgtcagaag 120 caaaagaaat aaaatcacag ttagagaacc aaaaagttaa atgggaacaa gagctctgca 180 gtgtgagatt gactttaaac caagaagaag agaagagaag aaatgccgat atattaaatg 240 aaaaaattag ggaagaatta ggaagaatcg aagagcagca taggaaagag ttagaagtga 300 aacaacaact tgaacaggct ctcagaatac aagatataga attgaagagt gtagaaagta 360 atttgaatca ggtttctcac actcatgaaa atgaaaatta tctcttacat gaaaattgca 420 tgttgaaaaa ggaaattgcc atgctaaaac tggaaatagc cacactgaaa caccaatacc 480 aggaaaagga aaataaatac tttgaggaca ttaagatttt aaaagaaaag aatgctgaac 540 ttcagatgac cctaaaactg aaagaggaat cattaactaa aagggcatct caatatagtg 600 ggcagcttaa agttctgata gctgagaaca caatgctcac ttctaaattg aaggaaaaac 660 aagacaaaga aatactagag gcagaaattg aatcacacca tcctagactg gcttctgctg 720 tacaagacca tgatcaaatt gtgacatcaa gaaaaagtca agaacctgct ttccacattg 780 caggagatgc ttgtttgcaa agaaaaatga atgttgatgt gagtagtacg atatataaca 840 atgaggtgct ccatcaacca ctttctgaag ctcaaaggaa atccaaaagc ctaaaaatta 900 atctcaatta tgccggagat gctctaagag aaaatacatt ggtttcagaa catgcacaaa 960 gagaccaacg tgaaacacag tgtcaaatga aggaagctga acacatgtat caaaacgaac 1020 aagataatgt gaacaaacac actgaacagc aggagtctct agatcagaaa ttatttcaac 1080 tacaaagcaa aaatatgtgg cttcaacagc aattagttca tgcacataag aaagctgaca 1140 acaaaagcaa gataacaatt gatattcatt ttcttgagag gaaaatgcaa catcatctcc 1200 taaaagagaa aaatgaggag atatttaatt acaataacca tttaaaaaac cgtatatatc 1260 aatatgaaaa agagaaagca gaaacagaaa actcatgaga gacaagcagt aagaaacttc 1320 ttttggagaa acaacagacc agatctttac tcacaactca tgctaggagg ccagtcctag 1380 cattacctta tgttgaaaaa tcttaccaat agtctgtgtc aacagaatac ttattttaga 1440 agaaaaattc atgatttctt cctgaagcct acagacataa aataacagtg tgaagaatta 1500 cttgttcacg aattgcataa aagctgccca ggatttccat ctaccctgga tgatgccgga 1560 gacatcattc aatccaacca gaatctcgct ctgtcactca ggctggagtg cagtgggcgc 1620 aatctcggct cactgcaact ctgcctccca ggttcacgcc attctctggc acagcctccc 1680 g 1681 181 432 PRT Homo sapien 181 Asp Thr Val His Ser Cys Glu Arg Ala Arg Glu Leu Gln Lys Asp His 1 5 10 15 Cys Glu Gln Arg Thr Gly Lys Met Glu Gln Met Lys Lys Lys Phe Cys 20 25 30 Val Leu Lys Lys Lys Leu Ser Glu Ala Lys Glu Ile Lys Ser Gln Leu 35 40 45 Glu Asn Gln Lys Val Lys Trp Glu Gln Glu Leu Cys Ser Val Arg Leu 50 55 60 Thr Leu Asn Gln Glu Glu Glu Lys Arg Arg Asn Ala Asp Ile Leu Asn 65 70 75 80 Glu Lys Ile Arg Glu Glu Leu Gly Arg Ile Glu Glu Gln His Arg Lys 85 90 95 Glu Leu Glu Val Lys Gln Gln Leu Glu Gln Ala Leu Arg Ile Gln Asp 100 105 110 Ile Glu Leu Lys Ser Val Glu Ser Asn Leu Asn Gln Val Ser His Thr 115 120 125 His Glu Asn Glu Asn Tyr Leu Leu His Glu Asn Cys Met Leu Lys Lys 130 135 140 Glu Ile Ala Met Leu Lys Leu Glu Ile Ala Thr Leu Lys His Gln Tyr 145 150 155 160 Gln Glu Lys Glu Asn Lys Tyr Phe Glu Asp Ile Lys Ile Leu Lys Glu 165 170 175 Lys Asn Ala Glu Leu Gln Met Thr Leu Lys Leu Lys Glu Glu Ser Leu 180 185 190 Thr Lys Arg Ala Ser Gln Tyr Ser Gly Gln Leu Lys Val Leu Ile Ala 195 200 205 Glu Asn Thr Met Leu Thr Ser Lys Leu Lys Glu Lys Gln Asp Lys Glu 210 215 220 Ile Leu Glu Ala Glu Ile Glu Ser His His Pro Arg Leu Ala Ser Ala 225 230 235 240 Val Gln Asp His Asp Gln Ile Val Thr Ser Arg Lys Ser Gln Glu Pro 245 250 255 Ala Phe His Ile Ala Gly Asp Ala Cys Leu Gln Arg Lys Met Asn Val 260 265 270 Asp Val Ser Ser Thr Ile Tyr Asn Asn Glu Val Leu His Gln Pro Leu 275 280 285 Ser Glu Ala Gln Arg Lys Ser Lys Ser Leu Lys Ile Asn Leu Asn Tyr 290 295 300 Ala Gly Asp Ala Leu Arg Glu Asn Thr Leu Val Ser Glu His Ala Gln 305 310 315 320 Arg Asp Gln Arg Glu Thr Gln Cys Gln Met Lys Glu Ala Glu His Met 325 330 335 Tyr Gln Asn Glu Gln Asp Asn Val Asn Lys His Thr Glu Gln Gln Glu 340 345 350 Ser Leu Asp Gln Lys Leu Phe Gln Leu Gln Ser Lys Asn Met Trp Leu 355 360 365 Gln Gln Gln Leu Val His Ala His Lys Lys Ala Asp Asn Lys Ser Lys 370 375 380 Ile Thr Ile Asp Ile His Phe Leu Glu Arg Lys Met Gln His His Leu 385 390 395 400 Leu Lys Glu Lys Asn Glu Glu Ile Phe Asn Tyr Asn Asn His Leu Lys 405 410 415 Asn Arg Ile Tyr Gln Tyr Glu Lys Glu Lys Ala Glu Thr Glu Asn Ser 420 425 430 

1. An isolated polypeptide comprising an immunogenic portion of a breast antigen or a variant thereof, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 2, 4-15, 18-33, 35-47, 49-56, 58, 59, 63-73, 88-116, 141-159, 175, 178 and 180; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions.
 2. The isolated polypeptide of claim 1, wherein the polypeptide comprises an amino acid sequence selected from the group consisting of SEQ ID NO: 62, 176, 179 and
 181. 3. An isolated polynucleotide comprising a nucleotide sequence encoding the polypeptide of claim
 1. 4. An isolated polynucleotide of claim 3, wherein the polynucleotide comprises a sequence provided in SEQ ID NO: 2, 4-15, 18-33, 35-47, 49-56, 58, 59, 63-73, 88-116, 141-159, 175, 178 or
 180. 5. An expression vector comprising a polynucleotide according to any one of claims 3 and
 4. 6. A host cell transformed with the expression vector of claim
 5. 7. The host cell of claim 6 wherein the host cell is selected from the group consisting of E. coli, yeast and mammalian cell lines.
 8. A pharmaceutical composition comprising the polypeptide of claim 1 and a physiologically acceptable carrier.
 9. A vaccine comprising the polypeptide of claim 1 and a non-specific immune response enhancer.
 10. The vaccine of claim 9 wherein the non-specific immune response enhancer is an adjuvant.
 11. A vaccine comprising a polynucleotide of any one of claims 3 and 4 and a non-specific immune response enhancer.
 12. The vaccine of claim 11 wherein the non-specific immune response enhancer is an adjuvant.
 13. A pharmaceutical composition for the treatment of breast cancer comprising a polypeptide and a physiologically acceptable carrier, the polypeptide comprising an immunogenic portion of a breast antigen, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 1, 3, 16, 17, 34, 48, 57, 60, 61, 74-87, 117-140 and 160-174; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions.
 14. A vaccine for the treatment of breast cancer comprising a polypeptide and a non-specific immune response enhancer, said polypeptide comprising an immunogenic portion of a breast antigen, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 1, 3, 16, 17, 34, 48, 57, 60, 61, 74-87, 117-140 and 160-174; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions.
 15. The vaccine of claim 14 wherein the non-specific immune response enhancer is an adjuvant.
 16. A vaccine for the treatment of breast cancer comprising a polynucleotide and a non-specific immune response enhancer, the polynucleotide comprising a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 1, 3, 16, 17, 34, 48, 57, 60, 61, 74-87, 117-140 and 160-174; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions.
 17. The vaccine of claim 16, wherein the non-specific immune response enhancer is an adjuvant.
 18. A method for inhibiting the development of breast cancer in a patient, comprising administering to the patient an effective amount of the pharmaceutical composition of claims 8 or
 13. 19. A method for inhibiting the development of breast cancer in a patient, comprising administering to the patient an effective amount of the vaccine of; any one of claims 9, 11, 14 or
 16. 20. A fusion protein comprising at least one polypeptide according to claim
 1. 21. A pharmaceutical composition comprising a fusion protein according to claim 20 and a physiologically acceptable carrier.
 22. A vaccine comprising a fusion protein according to claim 20 and a non-specific immune response enhancer.
 23. The vaccine of claim 22 wherein the non-specific immune response enhancer is an adjuvant.
 24. A method for inhibiting the development of breast cancer in a patient, comprising administering to the patient an effective amount of the pharmaceutical composition of claim
 21. 25. A method for inhibiting the development of breast cancer in a patient, comprising administering to the patient an effective amount of the vaccine of claim
 22. 26. A method for detecting breast cancer in a patient, comprising: (a) contacting a biological sample obtained from the patient with a binding agent which is capable of binding to a polypeptide, the polypeptide comprising an immunogenic portion of a breast antigen, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences, and sequences that hybridize to a sequence provided in SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions; and (b) detecting in the sample a polypeptide that binds to the binding agent, thereby detecting breast cancer in the patient.
 27. The method of claim 26 wherein the binding agent is a monoclonal antibody.
 28. The method of claim 26 wherein the binding agent is a polyclonal antibody.
 29. A method for monitoring the progression of breast cancer in a patient, comprising: (a) contacting a biological sample obtained from the patient with a binding agent that is capable of binding to a polypeptide, said polypeptide comprising an immunogenic portion of a breast antigen, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences and sequences that hybridize to a sequence provided in SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions; (b) determining in the sample an amount of a protein or polypeptide that binds to the binding agent; (c) repeating steps (a) and (b); and (d) comparing the amount of polypeptide detected in steps (b) and (c) to monitor the progression of breast cancer in the patient.
 30. A monoclonal antibody that binds to a polypeptide comprising an immunogenic portion of a breast antigen or a variant of said antigen, wherein said antigen comprises an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of: (a) nucleotide sequences recited in SEQ ID NO: 2, 4-15, 18-33, 35-39, 40-47, 49-56, 58, 59, 63-73, 88-116, 141-159, 175, 178 and 180; (b) complements of said nucleotide sequences; and (c) sequences that hybridize to a sequence of (a) or (b) under moderately stringent conditions.
 31. A method for inhibiting the development of breast cancer in a patient, comprising administering to the patient a therapeutically effective amount of a monoclonal antibody according to claim
 30. 32. The method of claim 31 wherein the monoclonal antibody is conjugated to a therapeutic agent.
 33. A method for detecting breast cancer in a patient comprising: (a) obtaining a biological sample from the patient; (b) contacting the sample with at least two oligonucleotide primers in a polymerase chain reaction, wherein at least one of the oligonucleotides is specific for a polynucleotide encoding a polypeptide comprising an immunogenic portion of a breast antigen, said antigen comprising an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences, and sequences that hybridize to a sequence of SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions; and (c) detecting in the sample a DNA sequence that amplifies in the presence of the oligonucleotide primers, thereby detecting breast cancer.
 34. The method of claim 33, wherein at least one of the oligonucleotide primers comprises at least about 10 contiguous nucleotides of a polynucleotide comprising a sequence selected from SEQ ID NO: 1-61, 63-175, 178 and
 180. 35. A diagnostic kit comprising: (a) one or more monoclonal antibodies of claim 30; and (b) a detection reagent.
 36. A diagnostic kit comprising: (a) one or more monoclonal antibodies that bind to a polypeptide encoded by a polynucleotide comprising a sequence selected from the group consisting of SEQ ID NO: 1, 3, 16, 17, 34, 48, 57, 60, 61, 74-87, 117-140 and 160-174, complements of said sequences, and sequences that hybridize to a sequence of SEQ ID NO:, 1, 3, 16, 17, 34, 48, 57, 60, 61, 74-87, 117-140 and 160-174 under moderately stringent conditions; and (b) a detection reagent.
 37. The kit of claims 35 or 36 wherein the monoclonal antibodies are immobilized on a solid support.
 38. The kit of claim 37 wherein the solid support comprises nitrocellulose, latex or a plastic material.
 39. The kit of claims 35 or 36 wherein the detection reagent comprises a reporter group conjugated to a binding agent.
 40. The kit of claim 39 wherein the binding agent is selected from the group consisting of anti-immunoglobulins, Protein G, Protein A and lectins.
 41. The kit of claim 39 wherein the reporter group is selected from the group consisting of radioisotopes, fluorescent groups, luminescent groups, enzymes, biotin and dye particles.
 42. A diagnostic kit comprising at least two oligonucleotide primers, at least one of the oligonucleotide primers being specific for a polynucleotide encoding a polypeptide comprising an immunogenic portion of a breast antigen, said antigen comprising an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences, and sequences that hybridize to a sequence of SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions.
 43. A diagnostic kit of claim 42 wherein at least one of the oligonucleotide primers comprises at least about 10 contiguous nucleotides of a polynucleotide having a sequence selected from SEQ ID NO: 1-61, 63-175, 178 and
 180. 44. A method for detecting breast cancer in a patient, comprising: (a) obtaining a biological sample from the patient; (b) contacting the biological sample with an oligonucleotide probe specific for a polynucleotide encoding a polypeptide comprising an immunogenic portion of a breast antigen, said antigen comprising an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences, and sequences that hybridize to a sequence of SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions; and (c) detecting in the sample a DNA sequence that hybridizes to the oligonucleotide probe, thereby detecting breast cancer in the patient.
 45. The method of claim 44 wherein the oligonucleotide probe comprises at least about 15 contiguous nucleotides of a polynucleotide comprising a sequence selected from the group consisting of SEQ ID NO: 1-61, 63-175, 178 and
 180. 46. A diagnostic kit comprising an oligonucleotide probe specific for a polynucleotide encoding a polypeptide comprising an immunogenic portion of a breast antigen, said antigen comprising an amino acid sequence encoded by a polynucleotide comprising a sequence selected from the group consisting of nucleotide sequences recited in SEQ ID NO: 1-61, 63-175, 178 and 180, complements of said nucleotide sequences, and sequences that hybridize to a sequence of SEQ ID NO: 1-61, 63-175, 178 and 180 under moderately stringent conditions.
 47. The diagnostic kit of claim 46, wherein the oligonucleotide probe comprises at least about 15 contiguous nucleotides of a polynucleotide comprising a sequence selected from the group consisting of SEQ ID NO: 1-61, 63-175, 178 and
 180. 48. A method for treating breast cancer in a patient, comprising the steps of: (a) obtaining peripheral blood cells from the patient; (b) incubating the cells in the presence of at least one polypeptide of claim 1, such that T cells proliferate; and (c) administering the proliferated T cells to the patient.
 49. A method for treating breast cancer in a patient, comprising the steps of: (a) obtaining peripheral blood cells from the patient; (b) incubating the cells in the presence of at least one polynucleotide of claim 3, such that T cells proliferate; and (c) administering to the patient the proliferated T cells.
 50. The method of any one of claims 48 and 49 wherein the step of incubating the T cells is repeated one or more times.
 51. The method of any one of claims 48 and 49 wherein step (a) further comprises separating T cells from the peripheral blood cells, and the cells incubated in step (b) are the T cells.
 52. The method of any one of claims 48 and 49 wherein step (a) further comprises separating CD4+ cells or CD8+ cells from the peripheral blood cells, and the cells proliferated in step (b) are CD4+ or CD8+ T cells.
 53. The method of any one of claims 48 and 49 wherein step (b) further comprises cloning one or more T cells that proliferated in the presence of the polypeptide.
 54. A composition for the treatment of breast cancer in a patient, comprising T cells proliferated in the presence of a polypeptide of claim 1, in combination with a pharmaceutically acceptable carrier.
 55. A composition for the treatment of breast cancer in a patient, comprising T cells proliferated in the presence of a polynucleotide of claim 3, in combination with a pharmaceutically acceptable carrier.
 56. A method for treating breast cancer in a patient, comprising the steps of: (a) incubating antigen presenting cells in the presence of at least one polypeptide of claim 1; and (b) administering to the patient the incubated antigen presenting cells.
 57. A method for treating breast cancer in a patient, comprising the steps of: (a) incubating antigen presenting cells in the presence of at least one polynucleotide of claim 3; and (b) administering to the patient the incubated antigen presenting cells.
 58. The method of claims 56 or 57 wherein the antigen presenting cells are selected from the group consisting of dendritic cells and macrophage cells.
 59. A composition for the treatment of breast cancer in a patient, comprising antigen presenting cells incubated in the presence of a polypeptide of claim 1, in combination with a pharmaceutically acceptable carrier.
 60. A composition for the treatment of breast cancer in a patient, comprising antigen presenting cells incubated in the presence of a polynucleotide of claim 3, in combination with a pharmaceutically acceptable carrier. 